Biomedical molding materials from semi-solid precursors
专利摘要:
The present invention relates to polymer moldings such as medical device moldings and to methods of making optical and ophthalmic lenses, preferably contact lenses and intraocular lenses. The invention also relates to polymer precursor mixtures and methods of making and using polymer precursor mixtures useful in polymer moldings. The semisolid polymerizable precursor mixture may comprise (i) a polymer blend consisting of two or more different prepolymers or one or more prepolymers and dead polymers; (ii) at least one non-reactive diluent; And (iii) optionally one or more reactive plasticizers. 公开号:KR20040015297A 申请号:KR10-2003-7016955 申请日:2002-06-26 公开日:2004-02-18 发明作者:마이클 알. 휴스톤;도시아끼 히노;데이비드 에스. 소안 申请人:지엠에스, 엘엘씨; IPC主号:
专利说明:
Biomedical Molding Materials from Semi-Solid Precursors {BIOMEDICAL MOLDING MATERIALS FROM SEMI-SOLID PRECURSORS} [2] Typically small moldings, such as contact lenses, were prepared by direct polymerization of liquid monomers. However, such materials have some problems. Liquids, for example, cause handling problems during mold filling, such as evaporation rings, bubble or pore formation, and the Schlieren effect. Sophisticated molds or methods must be used to keep the liquid in place until curing is complete. In addition, liquid materials typically act quickly to corrode or solvate the materials that come into contact with them when filled into the mold. Therefore, the mold could only be used once. In addition, the curing time of the liquid is too long and the molding shrinks considerably upon curing so that the molding does not accurately replicate the shape of the mold cavity. It is also difficult to provide additional surface properties to the moldings such as UV protection, dyes and the like. In addition, tedious extraction treatments are often required to immerse the mold in water or other non-toxic liquids for extended periods of time, usually several hours, to ensure biocompatibility and stability of the biomedical device. Residual toxic substances are removed by diffusion, which proceeds slowly. [3] Polymer products can be produced by injection molding, compression molding, or the like of a polymer resin. However, these techniques require high processing temperatures and are therefore not suitable for processing thermal sensitive polymers such as high refractive index polymers useful for ophthalmic lenses. [4] Summary of the Invention [5] The present invention relates to a method for producing moldings, in particular medical device moldings, more particularly optical lens moldings and ophthalmic lens moldings. Preferred moldings are contact lenses and intraocular lenses. Other examples of moldings that can be applied are biomedical moldings such as bandages or wound wrap devices, heart valves, coronary stents, artificial tissues and organs, and films and membranes. The moldings of the present invention may comprise drugs and / or therapeutic ingredients which are released from the molding in a controlled manner. This method uses a novel semisolid precursor mixture which is molded in a mold, cured and released from the mold to produce the desired molding. Another aspect of the invention relates to moldings prepared with the semisolid precursor mixtures used in the process of the invention. These aspects of the present invention and some preferred embodiments will be described in more detail below. [6] More specifically, an aspect of the present invention provides a polymer blend comprising (i) a polymer blend consisting of two or more different prepolymers or one or more prepolymers and dead polymers; (ii) at least one non-reactive diluent; And (iii) optionally at least one reactive plasticizer. The precursor mixture exhibits low shrinkage upon polymerization. [7] In addition, the semisolid polymerizable precursor mixture of the present invention is optionally molded into the desired form and exposed to the surface modification composition to obtain a semisolid gradient composite material exhibiting desirable surface properties. The precursor mixtures of the present invention may also contain active ingredients such as drugs and / or therapeutic ingredients, which are controlled release from the final molding. In a preferred embodiment of the present invention, polymerizing the semisolid precursor mixture provides an optically clear molding. [8] In another aspect, the present invention provides a novel process for forming a semi-solid precursor material, molding to take dimensions defined by a cavity of a mold, curing with a polymerization energy source, and releasing from the mold to produce the desired molding. It is about. An advantage of the novel process of the present invention is the rate of cure of the semisolid precursor mixture. As explained in more detail below, the total concentration of reactive species is very low in the semisolid precursor mixtures of the present invention. Therefore, the desired reactivity can be achieved very quickly (ie, can be cured quickly) and exhibit low shrinkage upon curing using the appropriate reaction initiator and source of polymerization energy. [9] "Quick cure time" and "quickly cured" means that the semisolid precursor mixture cures more quickly than the liquid composition where the liquid formulation has the same type of reactive functional groups and other curing parameters, such as constant energy strength and part morphology. Means that. Typically when using a photoinitiator a polymer energy source exposure time of about 10 minutes or less is needed to achieve the desired degree of cure. More preferably, curing is caused by exposure of less than about 100 seconds, more preferably exposure of less than about 10 seconds. Most preferably, a curing machine is caused when exposed to a polymerization energy source for less than about 2 seconds. Such a short cure time can be more easily realized in thin moldings such as contact lenses. [10] In another embodiment, the present invention also relates to an article having a surface and an inner center, wherein the composition of the surface material is distinguished from the composition of the central material, but at the same time a complete unit with the surface and the center integral. In the present invention, the semisolid polymer precursor mixture is optionally molded into the desired form and exposed to the surface modification composition to obtain a semisolid polymerizable gradient composite material, which is then shaped into a final molding and cured. [11] Therefore, the present invention provides a polymer blend comprising (a) an initiator and (i) at least two different prepolymers or at least one prepolymer and a dead polymer; (ii) at least one non-reactive diluent; And (iii) optionally mixing together a polymer precursor mixture comprising at least one reactive plasticizer and / or active ingredient to form a semisolid polymerizable composition exhibiting low shrinkage upon polymerization; (b) optionally forming the semisolid polymerizable composition into a preform of the desired form; (c) optionally exposing the preform to a surface modification material to form a semisolid gradient composite material; (d) introducing a semisolid polymerizable composition or semisolid gradient composite material into a mold of the desired form; (e) compacting the mold such that the semi-solid polymerizable composition or semi-solid gradient composite material takes the form of a mold internal cavity; (f) exposing the semisolid polymerizable composition or semisolid gradient composite material to a polymerization energy source; A method of making a molding comprising obtaining a cured molding, such as a molded optical lens or other medical device. This reaction is characterized by short curing times and low shrinkage upon curing. [1] The present invention relates to polymer moldings such as medical device moldings and to methods of making optical and ophthalmic lenses, preferably contact lenses and intraocular lenses. The invention also relates to polymer precursor mixtures and polymer precursor mixtures and methods of making and using the moldings useful for the production of polymer moldings. [12] As used herein in the specification and in the claims, the singular terms mean “one or more”. In one embodiment of the invention, the semisolid precursor mixture comprises a polymer blend comprising two or more types of polymerizable group containing prepolymers and a non-reactive diluent. The polymerizable group of the first prepolymer may be selected to be reactive or nonreactive with respect to the polymerizable group of the second prepolymer. If the first polymer cannot be reacted with the second polymer, the precursor mixture forms an interpenetrating polymer network (IPN) in which different prepolymers are independently crosslinked upon curing. If the first prepolymer can react with the second prepolymer, the precursor mixture forms a semi-interpenetrating polymer network wherein the different prepolymers crosslink together to form a single polymer network. [13] In another embodiment of the invention, the semisolid precursor mixture comprises a prepolymer, a dead polymer and a non-reactive diluent comprising a polymerizable group. Upon curing, the final product takes the form of a semi-interpenetrating polymer network comprising a crosslinked prepolymer network comprising a dead polymer and a non-reactive diluent. [14] In this embodiment without monomeric reactive species, the reaction proceeds only to the extent necessary to impart the desired mechanical properties to the final gel, which is generally a strong function of the crosslink density. When water-soluble, semi-solid prepolymer mixtures are used, the reaction should also be sufficient to make the resulting gel water insoluble if the molding is to be used in an aqueous environment. Therefore, the curing step can be completed quickly and efficiently since only a slight overall reaction is required when using a semisolid precursor mixture. In addition, since there are no small molecule monomers in this particular embodiment, there is no need to worry about unreacted monomers at the end of curing unlike conventional polymerization methods, and as compared with current state of the art methods involving monomer reactions. Curing time becomes short. [15] In another preferred embodiment of the present invention, the semisolid polymerizable precursor mixture is first formed and shaped into the desired form and then exposed to a surface modifying composition that may be reactive to obtain a semisolid gradient composite material. The surface modification composition is chosen such that the desired properties such as hydrophilicity or biocompatibility can be imparted to the surface of the final product. Since the semisolid precursor composition does not cure at this point in the method, the surface modified composition penetrates well into the central material and diffuses. The degree of surface modification can be controlled by adjusting the amount of surface modification composition applied to the core material, the hardness or density of the core material, and the miscibility between the core material and the surface modification composition. The semi-solid gradient composite material formed is molded and cured into a final product, wherein the surface material is distinct from the composition of the central material, but at the same time the surface and the center are all integral entities in which the surface layer is well adhered to the central material. Therefore, a novel and improved method for imparting desirable surface properties to a final cured product using the semisolid polymerizable composition of the present invention is provided. A more detailed description of semisolid gradient composite materials is described in WO 00/55653, which is incorporated by reference. [16] Another advantage of the methods disclosed herein is that when the free radical based polymerization process is used to cure the semisolid precursor mixture, the inhibitory effect due to oxygen is reduced. Without wishing to be bound by theory, it is believed that this effect is caused because the oxygen mobility inside the semisolid material before and during curing is lower than in conventional liquid substrate casting systems. Therefore, the complex and expensive methods currently used to exclude oxygen (used for both molding of moldings and molding of final parts, for example described in US Pat. Nos. 5,922,249 and 5,753,150) are used in the molding process. It may be omitted and the reaction may be completed in time in the manner described above. [17] Another advantage of the above-described invention is that the use of semisolid precursor mixtures avoids the usual liquid handling problems during mold filling, such as the inclusion of evaporation rings, bubbles or voids, and the sullene effect. In addition, there is less concern about the miscibility between the mixture and the mold material as semisolid materials do not have a rapid action to corrode or solvate the materials that typically come into contact with the mold. These advantages can be attributed to the properties of the semisolid material that the semisolid material has a weak solvation power even when small molecule species are present. While not wishing to be bound by theory, it is believed that this effect is due to the affinity for the semisolid matrix of any small molecule species present, such affinity inhibits or at least delays the migration of small molecules out of the semisolid material, thereby evaporating effects and mold materials. Delay or prevent corrosion of adjacent materials such as [18] It is therefore possible to use a wide range of suitable mold materials for forming the desired moldings according to the invention. Suitable mold materials may include quartz, glass, sapphire and various metals. Suitable mold materials may also be molded into optical quality surfaces and may include any thermoplastic material having mechanical properties that enable the mold to maintain its critical dimensions under the process conditions used in the methods disclosed herein. Examples of suitable thermoplastics include polyolefins such as low, medium, high-density polyethylene; Polypropylene and copolymers thereof; Poly-4-methylpentene; polystyrene; Polycarbonates; Polyacetal resins; Polyacrylic ethers; Polyarylether sulfones; Nylons such as nylon 6, nylon 11 or nylon 66; Polyester; And various fluorinated polymers such as fluorinated ethylene propylene copolymers. [19] Since semi-solid materials do not corrode the mold materials used to make the lenses well, significant processing advantages can be realized in recycling or reusing the lens mold after each molding cycle. Such reuse is facilitated by minimal reaction between the semisolid material and the mold material during the normal processing path, perhaps further facilitated by the rapid curing possible by the novel properties of the semisolid precursor material. Therefore, one embodiment of the present invention is that the contact lens mold is reused for one or more molding cycles by the use of the semisolid precursor mixture described herein, and a cleaning step is optionally performed between uses. [20] The invention also relates to novel semisolid precursor mixtures that can be used to prepare the desired moldings. The precursor mixture includes a polymerizable group that, upon curing, forms a polymer chain or polymer network. Polymerization mechanisms that may be mentioned herein by way of example only include free radical polymerization, cationic or anionic polymerization, cycloaddition, Diels-Alder reaction, ring open interchange polymerization and vulcanization. The polymerizable groups may be incorporated into the semisolid precursor mixture in the form of monomers, oligomers, as suspended reactive groups in the polymer backbone, or in the form of other reactive monomers, oligomers or polymer components. An oligomer or polymer having a reactive group or reactive is hereinafter referred to as "prepolymer". For the purposes of the present invention, a prepolymer is also referred to as a molecule having a formula weight of greater than 300, or a molecule comprising one or more repeating units linked together. Functionalized molecules having a formula weight of less than 300 and having only one repeat unit are referred to below as "reactive plasticizers". The prepolymer may have terminal and / or suspended reactive functional groups or may be prone to grafting or other reactions in the presence of the polymerization system used to construct the semisolid precursor mixture. The semisolid precursor mixture of the present invention comprises one or more prepolymers. [21] The semisolid precursor mixture may further comprise a non-reactive or substantially non-reactive polymer, referred to below as a "dead polymer." The dead polymer can act to add volume to the semisolid precursor mixture without adding a significant amount of reactive groups or the dead polymer can be selected to impart various chemical, physical and / or mechanical properties to the desired moldings. Dead polymers can also be used to impart the desired degree of semisolid consistency to the semisolid precursor mixture. Since the preparation of the desired prepolymer is expensive, it is also possible to use dead polymers to reduce the material cost of the semisolid precursor mixture. [22] Dead polymers that are miscible with the prepolymer can be chosen so that the final cured product can be homogeneous and optically transparent. It is also possible to select dead polymers that are immiscible with the prepolymer such that the cured final product comprises a phase separation mixture that exhibits the desired phase shape. For precursor mixtures comprising immiscible pairs of dead polymers and prepolymers, it is possible to obtain optically transparent phase-separated iso-refractive index articles having the same refractive indices in the dead polymer rich phase and the prepolymer rich phase in the final cured product. Phase-separated isorefractive index articles may also be formed from precursor mixtures comprising a mixture of immiscible prepolymers. If the semisolid precursor mixture of the present invention comprises only one type of prepolymer, the precursor mixture comprises one or more dead polymers. [23] In addition, the semisolid precursor mixtures of the present invention also include non-reactive or substantially non-reactive diluents. Diluents can act as extenders that do not contribute to the reactivity of the system or as admixtures that reduce the tendency of phase separation of other components in the mixture. If desired, the amount of non-reactive diluent may be selected to provide for the exchange of saline with saline after molding. Such molding methods are particularly useful for the manufacture of contact lenses that exhibit little or no expansion or contraction when placed in the curing and saline solution. Eastern blood casting allows for the manufacture of articles that accurately replicate the mold form upon curing and equilibration in the desired medium, such as physiologically acceptable saline. Although the diluent may play some role in the polymerization process, it is typically assumed to be non-reactive and have little effect on the polymer chains or networks formed upon polymerization. [24] In addition, small molecule reactive species (ie, monomers having a formula weight of less than about 300) may optionally add reactivity to the prepolymers, dead polymers, and non-reactive diluents of the semisolid precursor mixture and / or to achieve desirable semisolid consistency and miscibility. Can be added, in which case the small molecule reactive species can act to plasticize the polymer component. Small molecule species can act as polymerization extenders, promoters or terminators during the reaction. Regardless of the semisolid precursor mixture and the ultimate effect on subsequent polymerization reactions, the components will be referred to below as "reactive plasticizers". [25] In total, the semisolid precursor mixture should comprise a polymer blend, which is composed of two or more different prepolymers or one or more prepolymers and dead polymers and a non-reactive diluent. Reactive plasticizers / monomers may optionally be added for the reasons described above. Thus achieving the desired semisolid consistency of the precursor mixture, the desired reactivity (including the effects on curing time and shrinkage), the final physical and chemical properties of the produced moldings and the phase morphology that may be homogeneous or heterogeneous, and the preferred molding such as the eastern casting The components are selected and the composition is adjusted to achieve the method. In the polymerization to form the cured resin, the phase shape of the precursor material before curing is fixed to obtain a composite exhibiting elevated morphological stability. [26] "Polymer blend" means a mixture of two or more different polymer molecules. When functionalizing a polymer to obtain a prepolymer, the non-functionalized polymer forming the prepolymer and the prepolymer is considered to be different. [27] In a preferred embodiment of the invention, the semisolid polymerizable composition comprises a crosslinkable prepolymer, a dead polymer, at least one non-reactive diluent and optionally at least one reactive plasticizer. Crosslinkable prepolymers and dead polymers are preferably "equivalent", ie they will have similarities in structure. For example, preferred mixtures are homopolymers of hydroxyethylmethacrylate (HEMA) and methacrylic acid (MAA) monomers as crosslinkable prepolymers (pHEMA-co-MAA) and HEMA as dead polymers. (pHEMA), wherein the two polymers have different but equivalent chemical structures. The preferred MAA content of the functionalized pHEMA-co-MAA is less than 10%, more preferably less than 5%. [28] In another preferred embodiment, the precursor mixture comprises functionalized pHEMA-co-MAA as the first crosslinkable prepolymer and functionalized pHEMA as the second crosslinkable copolymer. [29] It is preferred that the non-reactive diluent is present in the semisolid precursor mixture in an amount that can provide for the exchange of eastern blood with the saline solution after molding. Preferred semisolid compositions formed are hydrophilic and water insoluble but water expandable, remain optically clear upon polymerization and equilibration in saline solution and exhibit low shrinkage or expansion. [30] "Semi-solid" means a mixture that is deformable and fusionable, but which can be treated as an integral, which can be fixed freely separately during short periods of operation, such as when inserted into a mold. In pure polymer systems, the elastic modulus of the pure polymeric material is approximately constant for molecular weights above a certain value known as fractional molecular weight. Therefore, for the purposes of the present invention and in one aspect of the present invention, semi-solids have an elastic modulus of up to a certain modulus of elasticity which is shown for pure polymer systems at high molecular weight, ie above fractional molecular weight, under fixed conditions such as temperature and pressure. It is defined as a substance to represent. Reduced modulus used to achieve semisolid consistency can be achieved by incorporating a plasticizer (reactive or non-reactive diluent) into the semisolid precursor mixture that acts to plasticize one or more prepolymers or dead polymer components. Alternatively, low molecular weight analogs below the fractional molecular weight for a given polymer (prepolymer or dead polymer) may be used in place of the fully polymerized form to achieve a reduction in modulus at processing temperatures. [31] Indeed, the semisolids referred to herein generally have a modulus of elasticity lower than about 10 10 -10 11 dyne / cm 2 . Whether the reduced elastic modulus of the semisolid at a given temperature is achieved by the reduction of the polymer (prepolymer or dead polymer) molecular weight or by the addition of reactive or non-reactive plasticizers, this is the preferred processing and final molding already mentioned above or detailed below. Provide the nature. [32] If the semisolid precursor mixture is cooled to achieve the desired semisolid consistency, one or more components of the solid precursor mixture may be frozen. See, for example, US Pat. No. 6,106,746. Therefore, for the purposes of the present invention and in another aspect of the present invention, the semisolid must also be defined as a material exhibiting an elastic modulus lower than the elastic modulus measured as its pure component in the frozen state of any of the frozen components. For example, if water is one of the components used in the semisolid precursor mixture and if the desired processing temperature is below 0 ° C. (freezing point of pure water), the mixture remains lower than pure, frozen water at its processing temperature. As long as it is considered semisolid. Therefore, the semisolid of the present invention will typically be distinguished from the frozen material because the elastic modulus of the semisolid material is kept below the elastic modulus of the pure component material exhibiting a freezing point temperature above the desired processing temperature. Such a decrease in elastic modulus is beneficial because the material halves are easier to deform when the metal halves are joined together to define the inner mold cavity and the shape of the molding. In addition, by choosing the semi-solid precursor composition wisely, the desired semi-solid consistency can generally be achieved near room temperature, thus realizing the advantages of handling when handling liquids and considerable cooling to realize the benefits of handling solids. No significant heating is required. [33] Semi-solids are distinguished from liquids in that they can be treated as separate freely fixed contents for at least the time required for the shortest processing operation. For example, insertion into a mold assembly would require handling the semisolid for about one second to recover a separate amount of semisolid material and place it on one half of the open mold. For this purpose, the semisolid can be in the form of a preform, where the semisolid has undergone a special preforming operation, and the conditions during and / or after the preforming operation can be adjusted to achieve semisolid consistency. Alternatively, semi-solid materials can be pumped from the container into the cavity mold using conditions such as not requiring a gasket or other mold enclosure to prevent material from flowing out of the mold too early. In contrast, liquids cannot be handled as separate freely fixed contents without unwanted flow and deformation even in the shortest processing steps. Gasket-sealed mold cavities or upright mold cavities with concave mold halves facing up should be used to prevent the liquid precursor mixture from flowing out of the mold in advance. This requirement is overcome in accordance with the present invention by using a unique semisolid precursor mixture that does not undesirably flow during short processing operations such as mold filling. [34] When heated, the temperature will have a strong effect on the flowability of the material because the semisolid material of the present invention will be significantly softened. If the semisolid material can be semisolid at least in part during the molding process, new uses of this material in the practice of the present invention are not excluded, although the semisolid may behave like a liquid upon sufficient heating. Indeed it was observed that materials exhibiting desirable semisolid consistency exhibited a viscosity of at least about 50,000 centipoise. In addition, the material was found to exhibit a dynamic modulus of at least 10 5 -10 6 dyne / cm 2 . These numbers were actually found not to represent absolute minimums for semisolid behavior but rather to indicate the approximate range in which semisolid behavior begins. [35] One advantage of the semisolid precursor mixtures of the present invention is the low shrinkage that can be realized upon curing. For example, considering the shrinkage upon curing of pure methyl methacrylate monomer, the shrinkage value given as the change in density during curing is approximately 25-30% (the specific gravity of the MMA monomer is -0.939 and the specific gravity of the PMMA is -1.19). to be). This shrinkage is due to the curing of the monomer, which has a methacrylate molar concentration of about 9.3 M (M = mol / liter). Larger molecular weight species exist, including up to oligomers, which can lower the methacrylate concentration to about 2-5 M and lower the shrinkage upon curing to about 7-15%. An advantage of using semisolid precursor mixtures in carrying out the present invention is that monomers with large concentrations of methacrylate groups (or other reactive functional groups such as acrylate, acrylamide, methacrylamide, vinyl, vinyl ether, allyl, etc.) And lower than the 2-5M level seen in oligomers, which was conventionally limited to the requirement of having a relatively low viscosity, ie, a viscosity sufficiently low to be processed as a liquid. Therefore, if the prepolymer is modified to have methacrylate functional groups at 1% in its backbone unit, the methacrylate concentration drops below about 1.0 M, resulting in shrinkage at approximately 0.3% of cure (shrinkage in this example system is It may actually be lower because the amount of shrinkage per methacrylate decreases qualitatively as the monomer size increases). Such low functional group concentrations could not be used by prior art methods because of the essential requirements of liquid-like low viscosity, which limits the size of reactive molecules that can be used for compounding purposes, leading to high potential shrinkage upon curing. . [36] Dilution of the prepolymer with a dead polymer and an inert plasticizer reduces the overall methacrylate concentration with the resulting shrinkage of the semisolid precursor mixture upon curing. Prepolymers containing few methacrylate groups can be mixed with dead polymers, non-reactive diluents and reactive plasticizers to obtain semisolid precursor mixtures that exhibit functional group concentrations of about 2 M or less and shrinkage upon curing of less than about 5%. This fact indicates that the monomers and prepolymers exhibit shrinkage of 15% and 1.0%, respectively, upon curing and are present in the semisolid precursor mixture at only 30% and 10% by weight, respectively, with the remainder being dead polymers and non-reactive diluents. It can be inferred considering that the expected shrinkage upon curing of the mixture will be approximately 4.6%. Therefore, for the purposes of the present invention, "low shrinkage" means that at least one of the following two conditions is met: (1) shrinkage measured by density change before and after curing is less than 5%; Or (2) the concentration of reactive groups prior to curing is less than 2M. A wide range of processing and blending advantages are possible, including the semisolid consistency of the precursor mixtures (as opposed to conventional liquid systems) disclosed by the present invention, which will be described in detail throughout this specification. [37] The semisolid precursor mixtures disclosed by the present invention can advantageously be used to form polymerizations and / or crosslinked products. Therefore, in another aspect, the present invention relates to moldings made by curing a semisolid precursor mixture. For the purpose of producing contact lenses or intraocular lenses, the moldings become hydrogels when placed in an essentially aqueous solution; That is, the composition of the molding is chosen such that it absorbs about 10 to 90% by weight of water when equilibrated in a pure aqueous environment but does not dissolve in aqueous solution. This molding is hereinafter referred to as "gel". [38] For the purposes of the present invention, essentially aqueous solutions include solutions comprising water as the main component, in particular aqueous salt solutions. Certain physiological salt solutions, ie saline solutions, may be preferably used to equilibrate or store the moldings instead of pure water. Particularly preferred aqueous salt solutions have an osmolality concentration of about 200 to about 450 millimolesmolal in 1 liter; More preferred solutions are in the range of about 250 to 350 millimoles / L. The aqueous salt solution is preferably a solution of physiologically acceptable salts such as phosphate salts known in the contact lens care art. The solution may further comprise an isotonic agent, such as sodium chloride, also known in the contact lens care art. Such solutions are generally referred to as saline solutions below, and salt solutions and compositions other than those currently known in the art of contact lens care are undesirable. [39] The moldings of the invention may advantageously be formed as contact lenses or intraocular lenses that exhibit “minimal expansion or contraction”, ie with little or no expansion or contraction of the gel when placed in saline solution. This can be achieved by adjusting the amount of non-reactive diluent present so that there is little change in the net volume of the gel when the molding is equilibrated in a saline environment. This is an exchange of eastern blood between the diluent and the saline solution. This object can be easily achieved by using saline as the sole diluent within the limits of incorporating saline into the semisolid precursor mixture at the same concentration as its equilibrium content after gel formation, the equilibrium content being readily determined by simple trial and error experiments. can do. If other diluents are to be used in the semisolid precursor mixture with or without saline, the diluent concentration that does not induce net volume changes of the gel when equilibrated with saline will not be the same as the equilibrium saline concentration, but is also facilitated by simple trial and error experiments. You can check it. [40] "Extraction" is the removal of unwanted or undesirable species (usually referred to as extractables, such as small molecule impurities, polymerization by-products, non-polymerized or partially polymerized monomers) from the cured gel prior to the intended use. "Before intended use" means before wearing on the eye, for example in the case of contact lenses. The extraction step is an essential step, for example in the prior art methods used to manufacture contact lenses (see US Pat. Nos. 3,408,429 and 4,347,198), which overly complicates the molding process and increases processing time and increases manufacturing costs. . [41] One advantage of the present invention is that once the polymerization step is completed, the molding can be produced without the need for an extraction step or with only a minimal extraction step. The "minimal extraction step" and "minimal extraction" are performed by fluid in a container in which the lens is packaged so that the amount of extractables is small (or low) and the extractable composition is sufficiently non-toxic so that any necessary extraction is delivered to the consumer It can be done. The expressions "minimal extraction step" and "minimal extraction" also include any washing or cleaning performed in part of any aspect of the release operation and any handling operation. That is, liquid jets are sometimes used to facilitate movement from one vessel of the lens to another, and to facilitate release from one or more lens molds, which generally comprise a stream of aimed water or saline solution. While it is expected that extraction or rinsing of any extractable lens material during these operations will be performed properly, any case should fall within the scope of materials and methods that require the minimum extraction steps described herein. [42] As an example, in one embodiment of the invention, the semisolid precursor mixture comprises 30-70% by weight prepolymer / dead polymer mixed with a photoinitiator, water and a non-reactive diluent selected from FDA-approved ophthalmic tackifiers. During polymerization, the molding can be placed directly into a contact lens packaging container containing about 3.5 mL of saline fluid for storage, with the aid of a liquid jet that aids in the release process and facilitates the handling of the lens by avoiding mechanical contact. See, for example, US Pat. No. 5,836,323) wherein the molding is equilibrated with the surrounding fluid in the package. Since the molding volume of the contact lens (e.g. -0.05 mL) is small relative to the fluid volume in the lens packaging, the viscosity of the glidant will be about 1% by weight or less for both the lens in solution and after equilibration, which is determined by the consumer. This is the concentration that can be applied directly to the eye. Therefore, although strictly an extraction step is used in this embodiment, the extraction step is reduced to the minimal extraction step that is potentially performed during release, handling and packaging methods. The fact that no separate extraction step is used represents itself an important advantage of the invention disclosed herein. [43] Substances and Methods [44] A prepolymer in which at least one site of the prepolymer chain of the invention is bonded via covalent bonds to the polymer backbone. In another embodiment, the present invention relates to a prepolymer that is not substantially water soluble. “Water soluble” means that the prepolymer may be dissolved in water or saline solution at a total concentration range of about 1-10% by weight of the prepolymer, or more preferably about 1-70% prepolymer, in water or saline solution under ambient conditions. It means that there is. Therefore, for the purposes of the present invention, "water insoluble" or "water insoluble" prepolymers should be those that are not completely soluble in water at a concentration range of about 1-10% in water at ambient temperature. In a preferred embodiment, the gel made from the water insoluble prepolymer may be water expandable to produce an optically clear homogeneous mixture when absorbing 10 to 90% of water. Generally such water expandable gels will exhibit maximum water absorption (ie, equilibrium water content) as a function of the chemical composition and gel crosslink density of the polymers making up the gel. Preferred gels according to the invention are those which exhibit an equilibrium water content of about 20 to 80% by weight in water or saline solution. Upon crosslinking, a water insoluble but water expandable material preferably forms a hydrogel which is a useful product of the present invention. [45] In a preferred embodiment of the present invention, the homogeneous semisolid precursor mixture according to the present invention is free of monomers, oligomers or polymer compounds (and by-products formed during the preparation of the prepolymer) used in the preparation of the prepolymer, And any other unwanted components such as impurities or diluents which are not present. "Substantially free" means that the concentration of undesirable components in the semisolid precursor mixture is preferably less than 0.001% by weight, more preferably less than 0.0001% (1 ppm). The acceptable concentration ranges for such undesirable components will ultimately be determined by the intended use of the final product. This mixture only contains a diluent that is approved by the FDA as an acceptable ophthalmic tackifier at limited concentrations in water or eyes. The mixture is also configured to contain no additional comonomer or reactive plasticizer. In this way the semisolid precursor mixture is configured to contain no or essentially unwanted components, and thus the moldings produced therefrom do not contain any or essentially unwanted components. After the cured molding has been produced, the molding is produced without requiring the use of a separate extraction step other than the extraction / equilibrium method performed in the packaging container and during the release and intermediate handling steps. [46] Prepolymers suitable for use in practicing the present invention include any thermoplastic material having one or more suspended or terminal functional groups (ie, reactive groups) along the oligomer or polymer backbone. In addition, oligomers or polymers that undergo graft reactions or other crosslinking reactions in the presence of a polymerization system (monomers, oligomers, initiators and / or polymerization energy sources) can be used as the prepolymer constituting the semisolid precursor mixture of the present invention. The prepolymers can be nanospheres or microspheres with linear, branched or lightly crosslinked polymers. [47] The functionalizing agent can be reacted with the polymer to introduce reactive groups into the polymer backbone to obtain the prepolymer. The reactive group may also be introduced onto the surface of the polymer nanospheres or microspheres to obtain a prepolymer. "Functionalizing agent" means a molecule having a group reactive to the polymer and introducing a reactive group into the polymer backbone upon reaction with the polymer. The functionalization reaction can be carried out as a single step using a suitable functionalizing agent. Or by reacting the functionalizable group on the polymer backbone with a molecule to another type of functionalizable group, which is then reacted with the functionalizing agent. Examples of functionalizable groups include, but are not limited to, hydroxyl, amines, carboxylates, thiols (disulfides), anhydrides, urethanes and epoxides. [48] Functionalizing agents for functionalizing polymers including hydroxyls include oxidation with hydroxyl-reactive groups such as epoxides and oxiranes, carbonyl diimidazoles, periodate, enzymatic oxidation, alkyl halogens, isocyanates, halohis Includes but is not limited to edible and anhydride. Functionalizing agents for functionalizing polymers comprising amine groups include amine-reactive groups such as isothiocyanates, isocyanates, acyl azides, N-hydroxysuccinimide esters, sulfonyl chlorides, aldehydes and glyoxals, epoxides And oxiranes, carbonates, arylating agents, amidoesters, carbodiimides, anhydrides and halohydrins. Examples of thio-reactive chemical reactions for functionalizing polymers comprising thiol groups include haloacetyl and alkyl halide derivatives, maleimides, aziridine, acryloyl derivatives, arylating agents, and thiol disulfide exchange reagents (such as pyridyl disulfides). Feed, disulfide reducing agent and 5-thio-2-nitrobenzoic acid). [49] Prepolymers suitable for the practice of the present invention are, for example: polystyrene, poly (α-methyl styrene), polymaleic anhydride, polystyrene-co-maleic anhydride, polystyrene-co-acrylonitrile, polystyrene-co-methyl ( Meth) acrylate, polymethyl (meth) acrylate, polybutyl (meth) acrylate, poly-iso-butyl (meth) acrylate, poly-2-butoxyethyl (meth) acrylate, poly-2- Methoxyethyl (meth) acrylate, poly (2- (2-ethoxy) ethoxy) ethyl (meth) acrylate, poly (2-hydroxyethyl (meth) acrylate), poly (hydroxypropyl (meth) Acrylate), poly (cyclohexyl (meth) acrylate), poly (isobornyl (meth) acrylate), poly (2-ethylhexyl (meth) acrylate), polytetrahydrofurfuryl (meth) acrylate , Polyethylene, polypropylene, polyisoprene, poly (1-butene), poly Butylene, Polybutadiene, Poly (4-methyl-1-pentene), Polyethylene-co- (meth) acrylic acid, Polyethylene-co-vinyl acetate, Polyethylene-co-vinyl alcohol, Polyethylene-co-ethyl (meth) acrylate , Polyvinyl acetate, polyvinyl butyral, polyvinyl butyrate, polyvinyl valerate, polyvinyl formal, polyethylene adipate, polyethylene azelate, polyoctadecene-co-maleic anhydride, poly (meth) acrylonitrile, Polyacrylonitrile-co-butadiene, polyacrylonitrile-co-methyl (meth) acrylate, poly (acrylonitrile-butadiene-styrene), polychloroprene, polyvinyl chloride, polyvinylidene chlorite, polycarbo Nate, polysulfone, polyphosphine oxide, polyetherimide, nylon (6, 6/6, 6/9, 6/10, 6/12, 11 and 12), poly (1,4-butylene adipate) Polyhexafluoropropylene jade Id, phenoxy resin, acetal resin, polyamide resin, poly (2,3-dihydrofuran), polydiphenoxyphosphazene, mono-, di-, tri-, tetra-, ... polyethylene glycol, Mono-, di-, tri-, tetra-, ... polypropylene glycol, mono-, di-, tri-, tetra-, ... polyglycerol, polyvinyl alcohol, poly-2 or 4-vinyl Pyridine, poly-N-vinylpyrrolidone, poly-2-ethyl-2-oxazoline, pyridine, pyrrole, imidazole, pyrazole, pyrazine, pyrimidine, pyridazine, piperdine, azolidine and morpholine Poly N-oxide, polycaprolactone, poly (caprolactone) diol, poly (caprolactone) triol, poly (meth) acrylamide, poly (meth) acrylic acid, polygalacturonic acid, poly (t-butylaminoethyl (Meth) atryl), poly (dimethylaminoethyl (meth) acrylate), polyethyleneimine, polyimidazoline, polymethyl vinyl ether, polyethyl vinyl ether , Polymethyl vinyl ether-co-maleic anhydride, cellulose, cellulose acetate, cellulose acetate butyrate, cellulose nitrate, methyl cellulose, carboxy methyl cellulose, ethyl cellulose, ethyl hydroxyethyl cellulose, hydroxybutyl cellulose, hydroxypropyl cellulose , Hydroxypropyl methyl cellulose, starch, dextran, gelatin, chitosan, polysaccharides / glucosides such as glucose and sucrose, polysorbate 80, zein, polydimethylsiloxane, polydimethyl silane, polydiethoxysilane, poly (Meth) acrylates-, (meth) acrylic anhydrides-, (meth) acrylamides of dimethylsiloxane-co-methylphenylsiloxanes, polydimethylsiloxane-co-diphenylsiloxanes, polymethylhydrosiloxanes, proteins, protein derivatives and synthetic polypeptides -, Vinyl-, vinyl ether-, vinyl ester-, vinyl halide-, non And silyl silane-, vinyl siloxane-, vinyl heterocycle-, diene-, allyl- and epoxy-functionalized forms. Ethoxylated and propoxylated forms of the polymers and copolymers thereof are also suitable for use as the prepolymer of the present invention. Other, less known but polymerizable functional groups can also be used, such as epoxides (with hardeners) and urethanes (reaction of isocyanates with alcohols). [50] In the present specification and claims, names such as "(meth) acrylate" or "(meth) acrylamide" are used to denote optional methyl substituents. In addition, the term "mono-, di-, tri-, tetra-, .... poly-" is used to refer to monomers, dimers, trimers, tetramers and the like up to a polymer comprising a given repeating unit. [51] Preferred prepolymers are polymers or copolymers comprising sulfoxide, sulfide and / or sulfone groups suspended in or inside the polymer backbone structure functionalized by additional reactive groups. Gels formed from sulfoxide-, sulfide- and / or sulfone containing monomers (without reactive groups added after initial polymerization) exhibited reduced protein adsorption in conventional contact lens formulations (US Pat. No. 6,107,365 and PCT). See WO 00/02937). It is readily incorporated into the semisolid precursor mixtures of the present invention. [52] In addition, preferred prepolymers are those which comprise one or more suspended or terminal hydroxyl groups, some of which are functionalized with reactive groups capable of undergoing free radical basic polymerization. Examples of such prepolymers are polyhydroxyethyl (meth) acrylate, polyhydroxypropyl (meth) acrylate, polyethylene glycol, cellulose, dextran, chitosan, glucose, sucrose, polyvinyl alcohol, polyethylene-co-vinyl Alcohols, mono-, di-, tri-, tetra-, .... functionalized forms of adducts of polybisphenol A and ε-caprolactone with C 2-6 alkane diols and triols. Copolymer, ethoxylated and propoxylated forms of such polymers are also preferred prepolymers (see, eg, PCT International Publication No. WO98 / 37441). [53] Copolymers of these polymers with other monomers and materials suitable for use as ophthalmic lens materials are also disclosed. Further monomers used in the copolymerization are for example without limitation vinyl lactams such as N-vinyl-2-pyrrolidone, (meth) acrylamides such as N, N-dimethyl (meth) acrylamide and diacetone (meth) Acrylamide, vinyl acrylic acid such as (meth) acrylic acid, acrylates and methacrylates such as 2-ethylhexyl (meth) acrylate, cyclohexyl (meth) acrylate, methyl (meth) acrylate, isobornyl (meth ) Acrylate, ethoxyethyl (meth) acrylate, methoxyethyl (meth) acrylate, methoxy triethylene glycol (meth) acrylate, hydroxytrimethylene (meth) acrylate, glyceryl (meth) acrylate Monomeric / backbone units, including dimethylamino ethyl (meth) acrylate and glycidyl (meth) acrylate, styrene and quaternary ammonium salts. [54] Particularly preferred prepolymers are methacrylate or acrylate functionalized poly (hydroxyethyl methacrylate-co-methacrylic acid) copolymers. The most preferred prepolymer is a copolymer of hydroxyethyl methacrylate with about 2% methacrylic acid, wherein about 0.2-5% of the suspended hydroxyl groups of the copolymer are functionalized with methacrylate groups to give a semisolid precursor mixture And reactive prepolymers suitable for the process of the invention are obtained. A more preferred degree of methacrylate functionalization is about 0.5-2% of hydroxyl. [55] In addition to the prepolymers, systems of interest in the present invention may include one or more substantially non-reactive polymer components, ie, dead polymers that can be linear, branched, or crosslinked. Dead polymers may also take the form of nanospheres or microspheres. The dead polymer can add volume to the semisolid precursor mixture without adding a significant amount of reactive groups, or the dead polymer can be selected to impart various chemical, physical, mechanical and / or morphological properties to the desired moldings. Dead polymers can also be used to impart the desired degree of semisolid consistency to the semisolid precursor mixture. If the preparation of the prepolymer is expensive, dead polymers can also be used to reduce the material cost of the semisolid precursor mixture. The dead polymer may be selected to be miscible or immiscible with the prepolymer. In one preferred embodiment of the invention, the composition of the dead polymer is equivalent to that of the prepolymer. [56] In the present invention, an optically transparent phase separation system can be advantageously prepared by including a prepolymer or a phase separation isoindex mixture of the prepolymer and the dead polymer. "Phase separation iso-refractive index" means a system that exhibits phase separation but maintains optical transparency because the refractive indices of coexisting phases are equal. When a non-reactive diluent and optionally a reactive plasticizer are added, it either (1) itself distributes almost equally to the phases or (2) has a refractive index similar to the polymer mixture upon polymerization, forming a transparent portion upon curing. Or if the non-reactive diluent and / or the reactive plasticizer itself are not equally distributed in the phases and do not have a refractive index similar to that of the polymer mixture upon curing, the refractive index of one of the phases can be varied by appropriate selection of the polymer composition to obtain an iso-refractive index mixture. have. According to the present invention, the above operations can be advantageously carried out to realize properties which have not previously been achieved (ie mechanical, optical and processing properties) for a given material system. [57] In the manufacture of optically transparent materials, virtually any thermoplastic material can be used as the dead polymer for the production of morphology-trapped materials. Examples include, but are not limited to, polystyrene, poly (α-methyl styrene), polymaleic anhydride, polystyrene-co-maleic anhydride, polystyrene-co-acrylonitrile, polystyrene-co- Methyl (meth) acrylate, polymethyl (meth) acrylate, polybutyl (meth) acrylate, poly-iso-butyl (meth) acrylate, poly-2-butoxyethyl (meth) acrylate, poly-2 -Ethoxyethyl (meth) acrylate, poly (2- (2-ethoxy) ethoxy) ethyl (meth) acrylate, poly (hydroxyethyl (meth) acrylate), poly (hydroxypropyl (meth) Acrylate), poly (cyclohexyl (meth) acrylate), poly (isobornyl (meth) acrylate), poly (2-ethylhexyl (meth) acrylate), polytetrahydrofurfuryl (meth) acrylate , Polyethylene, polypropylene, polyisoprene, poly (1-butene), polyisobutylene, polybutadiene, poly (4-methyl-1-pentene), polyethylene-co- (meth) acrylic acid, polyethylene-co-vinyl acetate, polyethylene-co-vinyl alcohol, polyethylene- Co-ethyl (meth) acrylate, polyvinyl acetate, polyvinyl butyral, polyvinyl butyrate, polyvinyl valerate, polyvinyl formal, polyethylene adipate, polyethylene azelate, polyoctadecene-co-maleic anhydride, Poly (meth) acrylonitrile, polyacrylonitrile-co-butadiene, polyacrylonitrile-co-methyl (meth) acrylate, poly (acrylonitrile-butadiene-styrene), polychloroprene, polyvinyl chloride, poly Vinylidene chlorite, polycarbonate, polysulfone, polyphosphine oxide, polyetherimide, nylon (6, 6/6, 6/9, 6/10, 6/12, 11 and 12), poly (1 , 4-butylene adipate), polyhexaple Oropropylene oxide, phenoxy resin, acetal resin, polyamide resin, poly (2,3-dihydrofuran), polydiphenoxyphosphazene, mono-, di-, tri-, tetra-, ... polyethylene Glycol, mono-, di-, tri-, tetra-, ... polypropylene glycol, mono-, di-, tri-, tetra-, ... polyglycerol, polyvinyl alcohol, poly-2 or 4 Vinyl pyridine, poly-N-vinylpyrrolidone, poly-2-ethyl-2-oxazoline, pyridine, pyrrole, imidazole, pyrazole, pyrazine, pyrimidine, pyridazine, piperdine, azolidine and Poly N-oxide, polycaprolactone, poly (caprolactone) diol, poly (caprolactone) triol, poly (meth) acrylamide, poly (meth) acrylic acid, polygalacturonic acid, poly (t-butyl) of morpholine Aminoethyl (meth) atryl), poly (dimethylaminoethyl (meth) acrylate), polyethyleneimine, polyimidazoline, polymethyl vinyl ether, poly Liethyl vinyl ether, polymethyl vinyl ether-co-maleic anhydride, cellulose, cellulose acetate, cellulose acetate butyrate, cellulose nitrate, methyl cellulose, carboxy methyl cellulose, ethyl cellulose, ethyl hydroxyethyl cellulose, hydroxybutyl cellulose, Hydroxypropyl cellulose, hydroxypropyl methyl cellulose, starch, dextran, gelatin, chitosan, polysaccharides / glucosides such as glucose and sucrose, polysorbate 80, zein, polydimethylsiloxane, polydimethyl silane, polydie Methoxysilane, polydimethylsiloxane-co-methylphenylsiloxane, polydimethylsiloxane-co-diphenylsiloxane, polymethylhydrosiloxane, proteins, protein derivatives and synthetic polypeptides. Ethoxylated and / or propoxylated forms of the polymers should also be included as dead polymers suitable for the present invention. [58] In one embodiment of the invention, preferred dead polymers are polymers or copolymers comprising sulfoxide, sulfide and / or sulfone groups contained within or suspended in the polymer backbone structure. Gels containing these groups exhibited reduced protein adsorption in conventional contact lens formulations (see US Pat. No. 6,107,365 and PCT International Publication No. WO 00/02937) and are readily incorporated into the semisolid precursor mixtures of the present invention. [59] Further preferred dead polymers are those comprising one or more suspended or terminal hydroxyl groups. Examples of such polymers are polyhydroxymethyl (meth) acrylate, polyhydroxypropyl (meth) acrylate, polyethylene glycol, cellulose, dextran, glucose, sucrose, polyvinyl alcohol, polyethylene-co-vinyl alcohol, mono -, Di-, tri-, tetra-, .... polybisphenol A and adducts of epsilon -caprolactone with C 2-6 alkane diols and triols. Copolymer, ethoxylated and propoxylated forms of such polymers are also preferred prepolymers. [60] Copolymers of these polymers with other monomers and materials suitable for use as ophthalmic lens materials are also disclosed. Further monomers used for the copolymerization of the dead polymers are, for example and without limitation, vinyl lactams such as N-vinyl-2-pyrrolidone, (meth) acrylamides such as N, N-dimethyl (meth) acrylamide and di Acetone (meth) acrylamide, vinyl acrylic acid such as (meth) acrylic acid, acrylates and methacrylates such as 2-ethylhexyl (meth) acrylate, cyclohexyl (meth) acrylate, methyl (meth) acrylate, iso Bornyl (meth) acrylate, ethoxyethyl (meth) acrylate, methoxyethyl (meth) acrylate, methoxy triethylene glycol (meth) acrylate, hydroxytrimethylene (meth) acrylate, glyceryl ( Monomer / backbone units including meth) acrylate, dimethylamino ethyl (meth) acrylate and glycidyl (meth) acrylate, styrene and quaternary ammonium salts. [61] The thermoplastic material may optionally have a small amount of reactive material attached to the polymer backbone (copolymerized, grafted or otherwise incorporated) to promote crosslinking upon curing. These may be amorphous or crystalline. These may be classified as high performance industrial thermoplastics (eg, polyether imides, polysulfones, polyether ketones, etc.), or they may be biodegradable natural polymers (eg, starch, prolamin and cellulose). Can be. These may naturally be oligomers or macromers. These examples do not limit the range of possible compositions in practicing the present invention, but merely illustrate the wide selection of thermoplastic chemistries allowed in the present invention. [62] Thermoplastic polymers have good optical transparency, high refractive index, low birefringence, exceptional impact resistance, thermal stability, UV transmittance or shielding resistance, tear resistance or burst resistance, desired degree of porosity, equilibrium in saline, Selective permeability (eg, high oxygen permeability), tissue compatibility, resistance to deformation, low cost, or a combination of these and / or other properties may be selected for the desired penetrant. [63] Polymer blends obtained by physically mixing two or more polymers are often used to provide the desired mechanical properties for a given material system. For example, impact modifiers (typically weakly crosslinked particles or linear polymer chains) may be mixed with various thermoplastics or thermoplastic elastomers to improve the impact strength of the final cured resin. Indeed the mixture may comprise a mechanical, latex or solvent-cast mixture; Graft type mixtures (surface modified grafts, occasional grafts (IPMs, mechanochemical mixtures)) or block copolymers. Depending on the chemical structure, molecular size and molecular structure of the polymer, this mixture may form a mixture comprising both miscible and immiscible, amorphous or crystalline components. [64] Most polymer blends and block copolymers and many other copolymers give rise to a phase separation system while providing a rich phase morphology used by material designers. The physical arrangement of the phase regions can be simple or complex and can represent continuous, separate / discontinuous and / or bicontinuous forms. Some of these are illustrated by the following examples: spheres of phase I dispersed in phase II; A cylinder of phase I dispersed in phase II; Interconnect cylinder; An aligned bicontinuous, double-diamond interconnect cylinder of phase I of phase II (documented as star block copolymer); Alternating lamellae (known as diblock copolymers of about the same chain length); A ring forming a nested spherical shell or helix; Phase inside phase (HIPS and ABS); And thermodynamics of phase separation (both nucleation and growth and spinoidal degradation mechanisms), simultaneous copies of these forms formed from the dynamics of the phase separation and methods of mixing, or combinations thereof. [65] Another range of materials uses "thermoplastic elastomers" as dead polymers or prepolymers (when functionalized). One example of a thermoplastic elastomer is a tri-block copolymer of the general structure "ABA", where A is a thermoplastic rigid polymer (ie, has a glass transition temperature higher than ambient temperature) and B is an elastomer (rubber) polymer (ambient temperature) Lower glass transition temperature). In the pure state, ABA forms a microphase separation or nanophase separation form. This form consists of the occlusion of the rigid glassy polymer region (A) connected and surrounded by the rubber chain (B), or the rubbery (B) surrounded by the glass (A) continuous phase. Depending on the relative amounts of (A) and (B) in the polymer, the form or structure of the polymer chain (ie linear, branched, star, asymmetric star, etc.), and the processing conditions used, alternating lamellas, semicontinuous rods Or other phase region structures can be observed in the thermoplastic elastomeric material. Under certain composition and processing conditions, the shape is such that the size of the relevant region is smaller than the wavelength of visible light. Therefore, the portion formed of the ABA copolymer can be transparent or even translucent in the worst case. Unvulcanized thermoplastic elastomers have rubber-like properties similar to conventional rubber vulcanizates, but flow like thermoplastics at temperatures above the glass transition temperature of the free polymer region. Examples of commercially available thermoplastic elastomers are SBS, SIS and SEBS, where S is polystyrene and B is polybutadiene, I is polyisoprene and EB is an ethylenebutylene copolymer. Many other diblock or triblock examples are known, such as poly (aromatic amide) -siloxanes, polyimide-siloxanes and polyurethanes. SBS and hydrogenated SBS (ie SEBS) are known products of Polymers Business, Kraton®. DuPont's Lycra® is also a block copolymer. [66] When thermoplastic elastomers are selected as starting prepolymers and / or dead polymers for the formulation, exceptionally impact resistant but transparent parts can be prepared by mixing with reactive plasticizers. The thermoplastic elastomer itself is not chemically crosslinked and requires a relatively hot processing step for molding. Upon cooling, such temperature fluctuations create dimensionally unstable, contracted or folded portions. If cured on its own, the reactive plasticizer can be chosen to form a relatively glassy rigid network or a relatively soft rubbery network, but in each case a relatively high shrinkage. However, when thermoplastic elastomers (i.e., dead polymers or prepolymers) and reactive plasticizers are mixed and reacted together to form cured resins, they have superior impact absorption and impact resistance properties and exhibit relatively small shrinkage during curing. Form a network. "Impact resistance" means resistance to breaking or breaking when impacting an incident object. [67] For use in ophthalmic and contact lenses, the prepolymers and dead polymers are selected such that the resulting polymerizable composition remains optically transparent upon polymerization and, in the case of contact lenses, upon equilibration in physiological saline. When the prepolymer and the dead polymer are mixed together in the polymerizable composition, they are generally selected to be compatible with each other so that an optically transparent lens is finally formed. Such miscible combinations are known in the art or can be determined without undue experimentation. In a preferred embodiment of the invention, the prepolymer and the dead polymer have equivalent chemical structures. It is also possible to produce optically transparent moldings by using the immiscible combinations of the prepolymer and the dead polymer to form the phase separation refractive index system as described above. [68] Depending on the nature of the prepolymers, dead polymers, nonreactive diluents and / or reactive plasticizers used in the formulation, the final cured resin may be more or less flexible (or more rigid or softer) than the starting prepolymer or dead polymer. . Composite articles that exhibit exceptional toughness can be made using thermoplastic elastomers which themselves contain polymerizable groups along the polymer chain. Preferred compositions for this can be, for example, SBS triblock or star copolymers, where the reactive plasticizer is believed to be weakly crosslinked with the unsaturated groups in the butadiene segment of the SBS polymer. [69] Preferred formulations for developing optically transparent and impact resistant materials use styrene-rich SBS triblock copolymers comprising up to about 75% styrene. These SBS copolymers are Kraton Polymers Business (Kraton®), Philips Chemical Company (K-Resin®), BASF (Styrolux®), Pina Fina Chemicals (Finaclear®), Asahi Chemical (Asaflex®), DENKA (Clearen®), and the like. In addition to high impact resistance and good optical clarity, the styrene-rich copolymer has a relatively high refractive index (ie, a refractive index of at least about 1.54) and / or a low density (less than 30% reactive plasticizer), so that the density is about 1.2 g / cc. Less than, more typically about 1.0 g / cc). [70] When mixture refractive index is a particularly important consideration, high refractive index polymers can be used as one or more dead polymer components. Examples of such polymers include polycarbonates and halogenated and / or sulfonated polycarbonates, polystyrenes and halogens and / or sulfonated polystyrenes, polystyrene-polybutadiene block copolymers and their hydrogenation, sulfonation and / or Halogenated forms (all of which may be linear, branched, star or asymmetric branched or star shaped, etc.), polystyrene-polyisoprene block copolymers and their hydrogenated, sulfonated and / or halogenated forms (linear, branched, Star and asymmetric branched and star forms, and the like), polyethylene or polybutylene terephthalate (or a variant thereof), poly (pentabromophenyl (meth) acrylate), polyvinyl carbazole, polyvinyl naphthalene, poly Vinyl biphenyl, polynaphthyl (meth) acrylate, polyvinyl thiophene, polysulfone, polyphenylene sulfide or oxide, polyphosphine oxide or Is a phosphine oxide containing polyether, urea-, phenol-, or naphthyl-formaldehyde resin, polyvinyl phenol, chlorinated or brominated polystyrene, poly (phenyl α- or β-bromoacrylate), polyvinylidene chloride or Bromine and the like. [71] In general, raising the aromatics content, halogen content (especially bromine) and / or sulfur content is known in the art as an effective way of raising the refractive index of the material. High refractive index, low density and impact resistance are particularly desirable for ophthalmic lenses that enable the manufacture of ultra-thin, light weight, spectacle lenses, which are desirable for their flat appearance and wearer comfort and safety. [72] Alternatively, elastomers, thermosets (e.g., uncured states such as epoxides, melamines, acrylated epoxies, acrylated urethanes, etc.) and other non-thermoplastic polymer compositions can be preferably used during the practice of the present invention. [73] In the present invention, a nonreactive diluent is advantageously added to the semisolid precursor mixture of the present invention in order to achieve miscibility of the mixture components, to achieve the desired concentration of reactive functional groups, and to achieve the desired desired semisolid consistency. Diluents are selected based on the miscibility and plasticity effects on the prepolymer and dead polymer components in the semisolid precursor mixture. "Mixable" refers to a thermodynamic state in which a non-reactive diluent solvates (solvates) or plasticizes prepolymers and dead polymers. In fact, molecular segments with similar structures were found to promote mutual dissolution. Therefore, the aromatic portion of the polymer is generally dissolved in the aromatic diluent and vice versa. Hydrophilicity and hydrophobicity are additional considerations in selecting prepolymers and dead polymers in non-reactive diluents and semisolid precursor mixtures. Miscibility can generally be estimated by systems that appear transparent at the time of mixing. However, for the purposes of the present invention, miscibility is not essential, but only preferred, especially where a transparent article is to be produced. Typically a miscible mixture is preferred for the production of the desired moldings, except where phase separation is unavoidable or desirable to achieve certain desired properties of the final molding. For ophthalmic and contact lens manufacture, transparent systems are preferred when cured, which can be easily achieved by selecting diluents that are miscible with the prepolymer and the dead polymer of the semisolid precursor mixture. [74] Diluents are substantially non-reactive in the polymerization system of semisolid precursor materials, but some reactions can occur in nature, and such reactions are generally acceptable and unavoidable. Diluents also act as chain terminators (e.g., a known phenomenon when water is present in the anionic polymerization system) and can reduce the rate of cure, the degree of final cure or the molecular weight distribution finally obtained. Fortunately, the semi-solid systems of the present invention require only a small amount of the overall reaction from the start to the end, as compared to the predominantly monomeric system, so that the interference effect of the diluent is also significantly reduced, often to the extent that the effects on the curing reaction cannot be observed. to be. This makes it very easy to select a diluent that can be used in the process of the present invention, since the reaction inhibition effect hardly occurs. [75] For example, non-reactive diluents include, but are not limited to: alcohols such as methanol, ethanol, propanol, butanol, pentanol and the like and methoxy and ethoxy ethers thereof; Glycols such as mono-, di-, tri-, tetra, ... polyethylene glycol and mono- and di-methoxy and -ethoxy ethers thereof, mono-, di-, tri-, tetra, ... Polypropylene glycol and its mono- and di-methoxy and -ethoxy ethers, mono-, di-, tri-, tetra, ... polybutylene glycol and its mono- and di-methoxy and -ethoxy Ethers, mono-, di-, tri-, tetra, ... polyglycerol and its mono- and di-methoxy and -ethoxy ethers; Alkoxylated glucosides such as ethoxylated and propoxylated glucosides described in US Pat. No. 5,684,058 and / or sold under the trade name “Glucam” by Amerchol Corp .; Ketones such as acetone, methyl ethyl ketone, methyl propyl ketone, methyl isobutyl ketone; Esters such as ethyl acetate or isopropyl acetate; Dimethyl sulfoxide, N-methylpyrrolidone, N, N-dimethyl formamide, N, N-dimethyl acetamide, cyclohexane, diacetone dialcohol, boric esters (e.g. glycerol, sorbitol or other multivalent compounds, US patent 4,495,313, 4,680,336 and 5,039,459). [76] Although the diluent used for the preparation of the desired molding is first extracted with a solvent other than water, and if desired, a second step of water extraction is carried out, the diluent used for the manufacture of contact lenses must ultimately be drainable. [77] The "unprescribed" use of viscous agents in ophthalmic compositions is regulated by the Food & Drug Adminstration (FDA) of the United States. For example, the federal treaty (21 CFR Part 349) of the title “Ophthalmic Drug Products for Over-the-Counter Use: Final Monograph” lists acceptable viscosity agents with appropriate concentration ranges for each. In particular, Sec. 349.12 describes the following classes of approved glidants: (a) cellulose derivatives: (1) carboxymethyl cellulose sodium, (2) hydroxyethyl cellulose, (3) hydroxypropyl methyl cellulose, methylcellulose ; (b) dextran 70; (c) gelatin; (d) polyols, liquids: (1) glycerin, (2) polyethylene glycol 300, (3) polyethylene glycol 400, (4) polysorbate 80, (5) propylene glycol; (e) polyvinyl alcohol; And (f) povidone (polyvinyl pyrrolidone). § 349.30 also suggests that up to three of the above glidants may be combined within the scope of this class. [78] The diluents used according to the invention are preferably FDA-approved ophthalmic tackifiers or mixtures of ophthalmic tackifiers with water or saline solutions. If water interferes with the polymerization process (which occurs less when using semi-solid mixtures than conventional polymerization processes using liquid monomer precursors), the neatness of the pure and / or viscous and prepolymers, dead polymers and / or reactive plasticizers Mixtures can be used. If the moldings must be diluted or equilibrated in water or saline solution before being used by the consumer, such as when contact lens moldings are packaged with excess saline for storage and transportation, the concentration of the viscous agent in the molding during curing is It may be much higher than the concentration approved by the FDA. [79] In a preferred embodiment of the invention, the diluent composition and concentration in the semisolid precursor mixture is chosen such that the net volume change of the gel volume is small during polymerization and subsequent equilibration in saline. Preferably the gel volume change is less than 10% upon equilibration in physiologically acceptable saline solution. More preferably, the gel volume change is less than 5%, even more preferably less than 2%. Most preferably the gel volume change is less than 1% when equilibrated in saline after molding, curing and releasing. [80] The minimum gel volume change when equilibrated in physiological saline is probably due to the novel semisolid precursor mixture of the present invention, where the semisolid material exhibits (1) low shrinkage upon curing and (2) the exact amount needed to replenish the equilibrium content of water. Because it can be formulated to contain an amount of diluent. The second condition is possible because the liquid system used in the conventional molding method is no longer required in the precursor mixture formulation. In contrast, the semi-solid consistency caused by incorporating the correct amount of diluent so that no gel volume change occurs upon equilibration in water is used as an advantage of the present invention. [81] In another preferred embodiment of the invention, the diluent concentration is adjusted to expand the fixed amount of gel upon equilibration in water. This sometimes helps the release method, which can be controlled by proper mold design, taking into account the expansion of a small but fixed amount of the final molding. [82] In the present invention, reactive plasticizers may optionally be included in the semisolid mixture. The reactive plasticizer is generally selected to be miscible with the remaining components of the desired precursor mixture, at least in the desired processing conditions of temperature and pressure. When curing is initiated using a reactive initiator, the additive mixture can be imparted by increasing the rate of fixing the phase form to the material immediately before curing to form a composite that exhibits elevated morphological stability. [83] The presence of non-reactive diluents and reactive plasticizers can lower the softening point of the polymer being mixed to promote mixing. This is particularly advantageous when temperature sensitive materials are mixed with high-Tg polymers. When an optically transparent material is desired, the mixture components (ie prepolymers, dead polymers, impact modifiers, non-reactive diluents and / or plasticizers) can be selected so that the refractive indices of the phases are the same (isotropy) so that light scattering is reduced. have. When the isorefractive index component is not available, the diluent and reactive plasticizer nevertheless serve as admixtures that help to reduce the size of the area between the two immiscible polymers below the optical wavelength so that the polymer mixture that is otherwise opaque is optically transparent. do. The presence of reactive plasticizers may also improve the adhesion between the impact modifier and the dead polymer in certain cases to improve the final mixture properties. [84] Even when only partial miscibility at room temperature is observed, a slight rise in temperature often results in a homogeneous mixture, ie many systems become transparent even with a slight rise in temperature. Such temperatures may extend to temperatures slightly above ambient or around 100 ° C. or higher. In such a case, the reactive component quickly cures at elevated temperature to “fix” the phase state that is miscible in the cured resin before the system is cooled. Therefore, phase trapping can be used to produce optically transparent materials instead of translucent or opaque materials that would otherwise form upon cooling, which is another advantage of the present invention. [85] In combination with non-reactive diluents, reactive diluents can be used alone or in mixtures to improve dissolution of a given prepolymer and dead polymer. The reactive functional groups can be acrylates, methacrylates, acrylic anhydrides, acrylamides, vinyls, vinyl ethers, vinyl esters, vinyl halides, vinyl silanes, vinyl siloxanes, (meth) acrylated silicones, vinyl heterocycles, dienes, allyls and the like. Other functional groups that are less known but polymerizable can also be used, such as epoxides (curing agents) and urethanes (reactions between isocyanates and alcohols). Although any monomer can in principle be used as a reactive monomer according to the invention, it is present as a liquid at ambient or slightly higher temperatures and can be polymerized easily and quickly by applying a polymerization energy source such as light or heat in the presence of a suitable initiator. Things are preferred. [86] Reactive monomers, oligomers and crosslinkers with acrylate and methacrylate functionalities are known and are commercially available from Sartomer, Radcure and Henkel. Similarly, vinyl ethers can be purchased commercially from Allied Signal / Morflex. Radcure also supplies UV curable cycloaliphatic epoxy resins. Vinyl, diene and allyl compounds can be purchased from many chemical suppliers. [87] To demonstrate the variety of reactive plasticizers that can be used to achieve such miscibility, some of the hundreds to thousands of commercially available compounds will be exemplified. For example, monovalent materials include, but are not limited to: butyl (meth) acrylate; Octyl (meth) acrylate; Isodecyl (meth) acrylate; Hexadecyl (meth) acrylate; Stearyl (meth) acrylate; Isobornyl (meth) acrylate; Vinyl benzoate; Tetrahydrofurfuryl (meth) acrylate; Caprolactone (meth) acrylates; Cyclohexyl (meth) acrylate; Benzyl (meth) acrylate; Ethylene glycol phenyl ether (meth) acrylates; Methyl (meth) acrylate; Ethyl (meth) acrylate; And propyl (meth) acrylates; Hydroxyethyl methacrylate (HEMA); 2-hydroxyethyl acrylate (HEA); Methylacrylamide (MMA); Methacrylamide; N, N'-dimethyl-diacetone (meth) acrylamide; 2-phosphatoethyl (meth) acrylate; Mono-, di-, tri-, tetra-, ... polyethylene glycol mono (meth) acrylate; 1,2-butylene (meth) acrylate; 1,3-butylene (meth) acrylate; 1,4-butylene (meth) acrylate; Mono-, di-, tri-, tetra-, penta-, ... polypropylene glymol mono (meth) acrylate; Glycerin mono (meth) acrylate; 4- and 2-methyl-5-vinylpyridine; N- (3- (meth) acrylamidopropyl) -N, N-dimethylamine; N- (3- (meth) acrylamidopropyl) -N, N, N-trimethylamine, 1-vinyl- and 2-methyl-1-vinylimidazole; N- (3- (meth) acrylamido-3-methylbutyl) -N, N-dimethylamine; N-methyl (meth) acrylamide; 3-hydroxypropyl (meth) acrylate; N-vinyl imidazole; N-vinyl succinimide; N-vinyl diglycolimide; N-vinyl glutarimide; N-vinyl-3-morpholinone; N-vinyl-5-methyl-3-morpholinone; Propyl meth (acrylate); Butyl meth (acrylate); Pentyl meth (acrylate); Dimethyldiphenyl methylvinyl siloxane; N- (1,1-dimethyl-3-oxobutyl) (meth) acrylamide; 2-ethyl-2- (hydroxy-methyl) -1,3-propanediol trimethyl (meth) acrylate; X- (dimethylvinylsilyl) -ω [(dimethylvinyl-silyl) oxy] -dimethyl diphenyl methylvinyl siloxane; Butyl (meth) acrylate; 2-hydroxybutyl (meth) acrylate; Vinyl acetate; Pentyl (meth) acrylates; Vinyl propionate; 3-hydroxy-2-naphthyl (meth) acrylate; Vinyl alcohol; N- (formylmethyl) (meth) acrylamide; 2-ethoxyethyl (meth) acrylate; 4-t-butyl-2-hydroxycyclohexyl (meth) acrylate; 2-((meth) acryloyloxy) ethyl vinyl carbonate; Vinyl [3- [3,3,3-trimethyl-1,1-bis (trimethylsiloxy) disiloxaneyl] propyl] carbonate; 4,4 '-(tetrapentacontmethylhepta-cosasiloxaneylene) di-1-butanol; N-carboxy-β-alanine N-vinyl ester; 2-methacryloylethyl phosphorylcholine; Methacryloxyethyl vinyl urea; Etc. [88] Multivalent materials include, but are not limited to: mono-, di-, tri-, tetra-, ... polyethylene glycol di (meth) acrylates; 1,2-butylene di (meth) acrylate; 1,3-butylene di (meth) acrylate; 1,4-butylene di (meth) acrylate; Mono-, di, tri-, tetra-, ... polypropylene glycol di (meth) acrylate; Glycerin di- and tri- (meth) acrylates; Trimethylol propane tri (meth) acrylate (and its ethoxylated and / or propoxylated derivatives); Pentaerythritol tetraacrylate (and its ethoxylated and / or propoxylated derivatives); Hexanediol di (meth) acrylate; Bisphenol A di (meth) acrylate; Ethoxylated (and / or propoxylated) bisphenol A di (meth) acrylates; (Meth) acrylated methyl glucoside (and its ethoxylated and / or propoxylated forms); (Meth) acrylated polycaprolactone triols in ethoxylated and / or propoxylated form thereof; Methylenebisacrylamide; Triallyl cyanurate; Divinyl benzene; Diallyl itaconate; Allyl methacrylate; Diallyl phthalate; Polysiloxaneylbisalkyl (meth) acrylates; Methacryloxyethyl vinyl carbonate; Polybutadiene di (meth) acrylate; And aliphatic and aromatic (meth) acrylic oligomers and (meth) acrylic urethane based oligomers of all kinds, such as Sartomer (SR series), Radcure (Ebecryl® series) and Henkel (Photomer® series). Typical crosslinkers usually, but not necessarily, have two or more ethylenically unsaturated double bonds. [89] Additional high hydrophilic monomers or comonomers useful in the present invention include, but are not limited to: acrylic acid; Methacrylic acid; (Meth) acrylamide- or meth (acrylate) -functionalized carbohydrate-, sulfoxide-, sulfide-, or sulfo based monomers such as those disclosed in US Pat. Nos. 6,107,365 and 5,571,882; Alkoxylated sucrose, glucose and other glucosides such as those disclosed in US Pat. Nos. 5,856,416, 5,690,953 and 5,654,350; N-vinylpyrrolidone; 2-acrylamido-2-methylpropanesulfonic acid and salts thereof; Vinylsulfonic acid and salts thereof; Styrenesulfonic acid and salts thereof; 3-methacryloyloxy propyl sulfonic acid and salts thereof; Allylsulfonic acid; 2-methacryloyloxyethyltrimethylammonium salt; N, N, N-trimethylammonium salts; Diallyl-dimethylammonium salts; 3-aminopropyl (meth) acrylamide-N, N-diacetic acid diethyl ester (as disclosed in US Pat. No. 5,779,943); Etc. [90] When a high refractive index material is desired, the reactive plasticizer can be selected to have a high refractive index, preferably to match the refractive indices of the prepolymers and dead polymers used. Examples of such reactive plasticizers in addition to those described above are brominated or chlorinated phenyl (meth) acrylates (eg pentabromo methacrylate, tribromo acrylate, etc.), brominated or chlorinated naphthyl or biphenyl ( Meth) acrylate, brominated or chlorinated styrene, tribromoneopentyl (meth) acrylate, vinyl naphthylene, vinyl biphenyl, vinyl phenol, vinyl carbazole, vinyl bromide or chloride, vinylidene bromide or chloride, bromoethyl (Meth) acrylate, bromophenyl isocyanate, and the like. As mentioned above, increasing the aromatic, sulfur and / or halogen content of reactive plasticizers is a known technique for achieving high refractive index properties. [91] In a preferred embodiment of the present invention, reactive plasticizers comprising acrylate, methacrylate, acrylamide and / or vinyl ether moieties have been found to form convenient, rapid curing UV-initiated systems. [92] The reactive plasticizer can be a mixture consisting of monovalent, divalent, trivalent or other multivalent materials. For example, incorporation of a mixture of monovalent and polyvalent reactive plasticizers results in the formation of reactive plasticizer polymer networks (ie, semi-IPNs) in which the reactive plasticizer polymer chains are crosslinked with one another during polymerization. During the polymerization, the growing reactive plasticizer polymer chain can be reacted with the prepolymer to form the IPN. Reactive plasticizers and prepolymers are also grafted or reacted with dead polymers (if present) to form IPNs when no unsaturated or other clearly reactive material is present in the dead polymer chain. Thus, the prepolymer and dead polymer chains can act as crosslinking materials during curing, forming a crosslinked reactive plasticizer polymer network even when only monovalent reactive plasticizers are present in mixture with the prepolymer and / or the dead polymer. have. [93] An initiator or polymerization catalyst is typically added to the semisolid precursor mixture to promote curing when the mixture is exposed to a polymerization energy source such as light or heat. The polymerization catalyst may be a thermal initiator that generates free radicals at appropriate elevated temperatures. Thermal initiators such as lauryl peroxide, benzoyl peroxide, dicumyl peroxide, t-butyl hydroperoxide, arobisisobutyronitrile (AIBN), potassium or ammonium persulfate are known for example and are Aldrich Can be purchased from a chemical supplier. Preferably, photoinitiators may be used in place of or in combination with one or more thermal initiators so that the polymerization reaction is initiated by a source of actinic or ionic radiation. Photoinitiators such as the Irgacure® and Darcour® families are known and commercially available from Ciba Geigy, and the Esacure® family can be purchased from Sartomer. Examples of photoinitiator systems include benzoyl methyl ether, 1-hydroxycyclohexyl phenyl ketone, 2-hydroxy-2-methyl-1-phenylpropan-1-one (trade name Darocure 1173 by Ciba Specialty Chemicals) Commercially available) and 4,4'-azobis (4-cyano valeric acid) available from Aldrich Chemicals. As a reference for the initiator, see, eg, Polymer Handbook, J. Brandrop, E.H. Immergut, eds., 3rd Ed., Wiley, New York, 1989. [94] Advantageously, the initiator can be added to the precursor mixture prior to introduction into the mold. Optionally other additives may also be included, such as release agents, preservatives, pigments, dyes, organic or inorganic fibers or granular reinforcement or extender fillers, thixotropic agents, indicators, inhibitors or stabilizers (weather or anti-yellowing agents), UV absorbers, interfaces Active agents, flow aids, chain transfer agents, blowing agents, porosity modifiers and the like. Initiators and other optional additives are dissolved or dispersed prior to combining with the dead polymer and / or prepolymer in the reactive plasticizer and / or diluent component to promote complete dissolution and uniform mixing into the polymer component (s). Alternatively, initiators and other optional additives may be added at any time, including just prior to polymerization, and may be preferred, for example when a thermal initiator is used. [95] The biomedical moldings of the invention can be used as a delivery system for the active ingredient which is carried out in a controlled release manner. Examples of active ingredients include, but are not limited to, drugs, pharmaceuticals, vaccines, antibiotics, genes and flavorings. When the prepolymer or dead polymer is present as nanospheres or microspheres, the active ingredient may be included or adsorbed on the nanospheres or microspheres. [96] In one embodiment of the present invention, contact lenses that also function as drug delivery systems are prepared from a semisolid precursor mixture comprising a prepolymer, drug-containing nanospheres or microspheres as a dead polymer, and an inert diluent. When the dead polymer is a drug containing microsphere, the precursor mixture can be advantageously formed as a phase separation iso-refractive system to improve the optical clarity of the contact lens. [97] In another embodiment of the present invention, a reusable drug release contact lens comprises a semipolymer precursor comprising a prepolymer, a dead polymer exhibiting affinity for the drug (which may be nanospheres or microspheres) and a non-reactive diluent Prepared from the mixture. The precursor mixture may be a homogeneous mixture or a phase separation isotropic system. The prepolymer is formed from a polymer that exhibits solubility properties that are sensitive to thermodynamic balances such as temperature, pH or ionic strength of physiologically acceptable aqueous solutions. When the contact lens is formed from a prepolymer exhibiting solubility characteristics that are sensitive to the temperature of the aqueous solution, the contact lens expands more at temperatures where the prepolymer is soluble than at temperatures where the prepolymer is insoluble. [98] For fluid mixtures, phase separation upon heating is referred to as the Lower Critical Solution Temparature (LCST) characteristic. Conversely, phase separation upon cooling is referred to as the Upper Critical Solution Temparature (UCST) characteristic. Polymers exhibiting LCST properties in aqueous systems include poly (N-isopropyl acrylamide), polyethylene glycol (PEG), polypropylene glycol (PPG), PEG-co-PPG copolymers and cellulose derivatives such as methyl cellulose derivatives . N-isopropyl acrylamide is also copolymerized with monomers comprising ionizable groups to obtain polymers that exhibit LCST properties depending on the pH and ionic strength of the solution. For aqueous solutions of PEG, LCST depends on the ionic strength of the solution. On the one hand, aqueous solutions of copolymers comprising N-acetyl acrylamide and acrylamide are known to exhibit UCST properties. LCST and USST observed in these systems are reversible. [99] Therefore, when the contact lens comprises a prepolymer formed from the LCST and UCST polymers and a dead polymer exhibiting affinity for the drug, the thermodynamic balance of the solution, such as temperature, causes the contact lens to expand and the drug to diffuse into the contact lens. The contact lens may be efficiently and repeatedly included in the contact lens by immersing the contact lens in a drug-containing solution that is adjusted to facilitate. The drug-containing contact lens produced in this way is immersed in the solution used for contact lens storage to restore the original lens shape. The formed drug-containing contact lens can be worn directly on the eye. [100] The components in the polymerization mixture can be mixed by manual mixing or by mechanical mixing. Preferably, the components may be slightly warmed to soften or liquefy the prepolymer and / or dead polymer components. Any suitable mixing device may be used to homogenize the mixture mechanically, such as mixers, kneaders, internal mixers, blenders, extruders, grinders, in-line mixers, electrostatic mixers, etc., optionally mixing at temperatures above ambient temperature, or Optionally at a pressure above or below atmospheric pressure. [101] In a preferred embodiment of the invention, there may be any waiting time for the components not to be mechanically stirred. Any such waiting time can be between the time the component is first metered into the holding vessel and the time of mechanical or manual homogenization. Alternatively, the ingredients may be metered into and added to the mixing device, and then the mixing device is operated for a sufficient time to "dry-mix" the ingredients, and then there may be any waiting time before further mixing. Alternatively, there may be a waiting time after the components have been thoroughly mixed in the mechanical device. The waiting time may be about 1 hour to 1 day or more. Such a waiting time is useful in achieving homogenization of the reduced polymer system, which has been reduced to very small lengths, since mechanical mixing techniques usually cannot achieve mixing in the microphase region length range. Therefore, the use of a combination of mechanical mixing and latency can achieve homogenization over all length ranges. The length of the waiting time as time to provide the most efficient overall mixing method in terms of energy consumption, overall process economics and final material properties and the order in the processing method can be selected empirically without undue experimentation. [102] Embodiments of the present invention are particularly advantageous when the polymerizable mixture comprises a high proportion of prepolymer or dead polymer component, especially when the prepolymer or dead polymer is glassy or hard at ambient temperature. It may also be particularly advantageous to utilize a wait time when the prepolymer and / or the dead polymer are thermally sensitive and cannot be processed without excessive degradation for a certain time at temperatures above their softening point. [103] When attempting to mix two or more polymers, it may be useful to plasticize by first adding a non-reactive diluent and / or a reactive plasticizer to the component at the highest glass transition temperature. Other components of lower Tg can be mixed at lower temperatures than can be used without the plasticizing effect of diluents or reactive plasticizers to reduce the overall thermal exposure of the system. Alternatively, diluents and reactive plasticizers can be dispensed into the polymers to be mixed so that each can be plasticized separately. Individually plasticized polymers can be mixed at relatively low temperatures, with lower energy consumption and polymer degradation to match. [104] An important criterion for determining whether the present invention for preparing ophthalmic moldings, such as contact lenses and spectacle lenses, can be used in the novel method is that the precursor mixture must be homogeneous enough to allow for optical clarity upon curing; The mixture should exhibit semisolid consistency during at least a portion of the manufacturing method used to produce the desired moldings; The mixture must be able to undergo a polymerization reaction when applying light, heat or certain other forms of polymerization energy or polymerization initiation mechanism; The mixture should exhibit low shrinkage upon polymerization. Additional preferred properties of the spectacle lens include one or more of the following: optical transparency to transmit at least 80%, preferably at least 85% and most preferably 90% of light in the visible spectrum range at 2 mm thickness; Refractive index of at least 1.5; Glass transition temperature of 80 ° C. or higher; Modulus of elasticity greater than 10 9 dyne / cm 2 ; Shore D hardness of greater than 80; And an Abbe value greater than 25. [105] The semisolid precursor materials of the present invention can be advantageously molded by several different molding techniques known and commonly performed in the art. For example, electrostatic casting techniques are known in the thermoplastic molding art that define the shape of the moldings that are made by placing the molding material in two mold halves and then closing it to define the mold cavity. See, for example, US Pat. Nos. 4,113,224, 4,197,226 and 4,347,198. Compression molding techniques are also known in the thermoplastic molding art that form two or more mold halves together without needing to be in contact with each other to form one or more surfaces. Injection molding is another technique that can be employed for the semisolid precursor material of the present invention, in which the semisolid material is quickly forced into a cavity defined by two temperature controlled mold halves, and then the material is removed from the mold. It is optionally cured and injected from the mold halves and, if necessary (if the semisolid is not cured or partially cured in the injection molding machine) a subsequent molding or curing step is performed. [106] Processes that do not cure in the mold or only partially cure are suitable for the production of preforms, which can be used in electrostatic casting or compression molding processes where cure is performed to produce the desired final product. Electrostatic casting, compression and injection molding are all preferred in the manufacture of ophthalmic lenses because of their predominance over non-reactive thermoplastics (injection and compression molding) or reactive thermoplastic precursors (electrostatic casting) in the liquid state. [107] If desired, the preform may be further exposed to a surface modification or surface forming material to obtain a semisolid gradient composite material that exhibits the desired surface properties. As used herein and in the claims, the terms "surface modifying material" and "surface active material" are used interchangeably and refer to any composition or material that adds or provides a layer with the desired properties to one or more surfaces of the polymeric article. do. Compositions useful for making the moldings of the present invention may be dye or pigment solutions, which may be photochromic, fluorescent, UV-absorbing or visible (color), if described. The dye may be included in, covalently bonded, adsorbed or immobilized on a carrier, such as a hyperbranched polymer, nanosphere, or microsphere, which may contain reactive groups. Or the surface composition may comprise a scratch resistant precursor formulation. In addition, the dye is dissolved directly in the scratch resistant material to produce the final product, such as a lens, which can be simultaneously shaded and scratched. Another example of a surface forming or surface modifying composition is a hydrophilic monomer / crosslinker mixture, such coatings provide, for example, hydrophilicity and / or tissue compatibility to contact lenses and antifog to spectacle lenses and windscreens. do. Such hydrophilic reactive monomer / crosslinker compositions may also further comprise various dyes including photochromic species. [108] The preform may be exposed to the surface forming composition by immersing it in a bath of the surface forming composition. In addition to immersing in the bath, the surface forming composition can be evaporated, painted, spun, printed, or electroformed onto the preform by methods known to those skilled in the art of coating and pattern formation / transcription. Alternatively, the surface forming composition can be sprayed, painted, printed, patterned, flow coated or applied to one or more surfaces of the mold. The surface forming composition may optionally be cured or partially cured to increase viscosity, toughness, wear resistance or other desirable properties. A more detailed description of semisolid gradient composite materials is disclosed in WO 00/55653, which is incorporated by reference. [109] Silicone-containing polymers are known to have high oxygen permeability but poor tissue compatibility. In one preferred embodiment of the invention, the preform is first formed from a semisolid precursor mixture comprising a silicone containing prepolymer and / or a dead polymer, and then the preform is exposed to a surface modified composition comprising a hydrophilic monomer. . Semisolid gradient composite materials obtained in this way are molded and cured into contact lenses, which exhibit high oxygen permeability and improved tissue compatibility. [110] The method of the present invention is advantageous over conventional molding techniques in which the semisolid precursor material is small, unlike liquid precursors used in electrostatic casting techniques, but provides finite flow resistance so that the semisolid material does not flow down when introduced into the mold. Because there is. The semisolid material is also flexible enough to easily compress and deform without undue resistance when combining the two electrostatic compression molds together to achieve the desired mold shape or surface properties. Furthermore, unlike typical thermoplastics, semisolid materials do not require excessive or undesirable amounts of heating and / or compressive forces typical of compression or injection molding using conventional materials. Therefore, the semi-solid materials of the present invention can be considered to be systems that can be cured with semi-IPN or crosslinked gels upon reactive (but low shrinkage) curing combined with the ease of deformation of liquids and the ease of handling of solids. [111] Thus, in one embodiment, the semisolid precursor material provides a thermoplastic like material that, unlike conventional thermoplastics, can be cured after molding to provide a crosslinking, thermoset system. If the semisolid system is excessively plasticized relative to the pure thermoplastics that make up the polymer formed by the polymerization of the prepolymers, dead polymers or reactive plasticizers used in the semisolid systems, the semisolids are advantageously easier and / or easier than those thermoplastics. Will flow at a lower temperature. [112] In another embodiment, the semisolid precursor material is a liquid in which the semisolid will not improperly flow out of the mold, can be cured quickly, and exhibits a small shrinkage relative to the liquid precursor analog when cured, without the oxygen inhibiting effect. Provides improvements over the precursor material system. [113] The polymerization of the semisolid precursor mixture in the mold granules is preferably carried out by exposing the mixture to polymerization initiation conditions. Cure times can often last from a few minutes to parts that are thermally cured, often by heating slightly above ambient temperature. Or, when free radical or cation cure mechanism is used and initiated by a high intensity UV light source, the cure may last from a few minutes to less than a few seconds. A preferred technique is to expose the photoinitiator containing composition to an ultraviolet (UV) radiation source at a strength and time sufficient to initiate the desired degree of polymerization. The polymerization will generally be carried out after the removal of the polymerization energy source, for example the UV light source, and the time required to effectively complete the polymerization to the desired degree can be determined without undue experimentation. If desired, relatively strong UV light can be used with the semisolid precursor mixture of the present invention to complete sufficient curing in a short time without excessive heat generation in the curing system. This advantage is particularly evident when the reactive species of the semisolid precursor mixture comprises only the prepolymer and optionally comprises a small amount (eg less than about 30% by weight, more preferably less than about 20% by weight) of one or more reactive plasticizers. Do. [114] Preferred embodiments according to the invention comprise the following steps: [115] a) a polymer blend comprising at least one prepolymer and a dead polymer; Non-reactive diluents; Photoinitiators; And introducing a semi-solid precursor material into the mold, the semi-solid precursor material comprising any reactive diluent; [116] b) initiating the photocrosslinking reaction for up to 1 minute with a polymerization energy source such as UV light; [117] c) open the mold and remove the cured molding; The cured moldings are placed in packaging for storage and / or transportation. [118] In another preferred embodiment, the semisolid precursor mixture is not water soluble (ie, not soluble in water in a concentration range of 1-10% by weight in water), but is preexpanded or prepolymer / dead expanded after curing. Polymer blends. The composition can be mixed with a viscous type diluent to avoid the need for a separate extraction step after curing in addition to being carried out in the release, handling and packaging of the formations made therefrom. [119] In a preferred embodiment of the invention, the semisolid precursor mixture comprises a water-insoluble but water-expandable prepolymer which is a functionalized copolymer of polyhydroxyethyl methacrylate (pHEMA). This copolymer may include methacrylic acid, acrylic acid, n-vinyl pyrrolidone, dimethylacrylamide, vinyl alcohol and other monomers with HEMA. Preferred embodiments include polymers of HEMA copolymerized with approximately 2% methacrylic acid. This copolymer may also include reactive dyes and / or reactive UV absorbers. These copolymers are then functionalized with methacrylate groups (or acrylate groups) to form reactive prepolymers suitable for the preparation of ophthalmic moldings useful as contact lenses. HEMA based copolymers can be functionalized via the hydroxyl groups of HEMA using, for example, methacrylate anhydride and glycidyl methacrylate. [120] In a preferred embodiment, the precursor mixture is a pHEMA-co-MAA copolymer as a prepolymer, pHEMA as a dead polymer, 1,2-propylene glycol as a non-reactive diluent and a 50:50 (weight) mixture of water and a water soluble photoinitiator such as 4 , 4'-azobis (4-cyanovaleric acid) (ACVA). The initiator concentration is approximately 0.5% by weight and the concentration of non-reactive diluent is approximately 50% by weight. A 50:50 mixture of PEG 400 or PEG 400: water can be used in place of the propylene glycol: water mixture. In another preferred embodiment, the precursor mixture is functionalized pHEMA-co-MAA copolymerized with functionalized pHEMA as first prepolymer, reactive dye as second prepolymer and reactive UV absorber, PEG 400 as non-reactive diluent And Irgacure 1750 as photoinitiator. [121] Upon mixing the material becomes a transparent, homogeneous semisolid precursor mixture. A small amount of semisolid precursor mixture is separated from the bulk mass and inserted into the mold cavity as individual quantities. Closing the mold deforms the semisolid and takes the form of an internal mold defined by the mold halves. When the sample is irradiated with a polymerization energy source such as UV light, the precursor mixture is cured into a water expandable crosslinked gel and then released and transferred to a saline solution for equilibration. This gel will be designed to absorb approximately 30-70% water when equilibrated but exhibit mechanical properties such as elongation-to-break and modulus similar to commercially available contact lens materials. The moldings thus prepared are therefore useful as ophthalmic lenses, in particular contact lenses or intraocular lenses, wherein the lenses are made of semisolid precursor materials which exhibit low shrinkage during the rapid curing step, the lenses being separate from the equilibrium step in packaging No extraction step is required. [122] Another preferred embodiment uses hydrophilic silicone, which is a copolymer of a hydrophilic component as a dead polymer and a silicone component exhibiting high oxygen permeability, or when used as a prepolymer or reactive plasticizer when having additional functional groups. Silicone based monomers and prepolymers suitable for incorporation into the semisolid precursor mixtures of the present invention are described in U.S. Pat.Nos. 4,136,250, 4,153,641, 47,405,33, 50,0,141, 50,344, 61, 50,575, 78, 5,702,5. Nos. 5336797, 5356797, 5371147, 5387632, 5451617, 5486579, 5789461, 5807944, 5962548, 5998498, 6020445 and 6031059 PCT Application WO 94/15980, WO 97/22019, WO 99/60048, WO 99/60029, WO 01/02881 and European Patent Application EP00940447, EP00940693, EP00989418 And EP00990668. [123] Another preferred embodiment uses perfluoroalkyl polyethers which are fluorinated for good oxygen permeability and inertness but exhibit an acceptable degree of hydrophilicity due to the polymer backbone structure and / or hydrophilic suspended groups. Such materials can be readily incorporated into the semisolid precursor mixtures of the present invention as dead polymers or as prepolymers or reactive plasticizers when they have additional functional groups. See US Pat. Nos. 5965631, 5973089, 6060530, 6160030, and 6225367 for examples of such materials. [124] Example 1 General Preparation of Functionalized pHEMA [125] 10 g of poly (2-hydroxyethyl methacrylate (pHEMA, MW = 300,000) was dissolved in anhydrous pyridine To this solution, 0.114 mL of methacrylate anhydride was added and the mixture was continued for 12 to 24 hours. The pyridine was removed in vacuo and the functionalized pHEMA was precipitated twice in water to remove impurities After drying, a 1% functional (theoretical) pHEMA was obtained, where 1% of the original hanging hydroxyl group Modified to have suspended methacrylate functional groups Compared to the pHEMA starting material used, this corresponded to about 20-25 suspended methacrylate groups per polymer chain. [126] Various degrees of functionality (range of 0.3% to 5%) of pHEMA were prepared according to the method described above. Different degrees of functionality were readily prepared by adjusting the amount of methacrylate added to the pHEMA-pyridine mixture. In addition, other reactive groups (eg, acrylate, (meth) acrylamide, etc.) could be attached to the pHEMA chain using similar methods. [127] Example 2: Preparation of Functionalized pHEMA-co-MAA [128] 150 mL of anhydrous pyridine was charged to a flask equipped with a reflux condenser, thermometer and nitrogen injection tube. 10 mL of 2-hydroxyethyl methacrylate (HEMA), 0.14 mL of methacrylic acid (MAA) and 15 mg of 2,2'-azobisisobutyronitrile were then added to the flask. After purifying the solution with nitrogen for 15 minutes, the solution was slowly heated to 70 ° C. and the polymerization reaction was initiated to synthesize pHEMA-co-MAA. [129] The polymerization was typically continued for 6-8 hours while the solution was cooled to room temperature. As the functionalizing agent, 0.12 mL of methacrylic anhydride was injected and the solution was stirred for 12 hours to introduce a reactive methacrylate group through the hydroxyl group of HEMA into the main chain of pHEMA-co-MAA. [130] The functionalization reaction was completed and the pyridine, residual monomers and impurities were removed by vacuum distillation to yield a functionalized pHEMA-co-MAA prepolymer. Non-reactive diluents such as ethanol and dead polymers such as pHEMA were mixed with the functionalized pHEMA-co-MAA prepolymer to obtain a semisolid precursor mixture that can be used directly for molding and curing. [131] Functionalized pHEMA-co-MAAs of different degrees of functionality were also prepared according to the methods described above. [132] Example 3: Preparation of pHEMA-co-MAA in the presence of a non-reactive diluent. [133] In this example, the functionalized pHEMA-co-MAA prepolymer was synthesized in a polymerization medium comprising a non-reactive diluent constituting the semisolid precursor mixture. [134] The reactor consisted of a temperature controlled 250 mL four neck flask equipped with a thermometer, condenser and nitrogen inlet. The reactor was charged with 10 g of average molecular weight 400 polyethylene glycol (PEG 400, Aldrich) as a non-reactive nonvolatile diluent and 20 g of acetone as volatile solvent. After stirring the mixture for several minutes, 10 g of 2-hydroxyethyl methacrylate (HEMA), 0.15 g of methacrylic acid (MAA) and 12 mg of azobisisobutyronitrile (AIBN) were added as an initiator. The mixture was clarified with nitrogen with stirring for approximately 15 minutes. [135] The solution was slowly heated and held at 60 ° C. for 2 hours to effect polymerization. After polymerization, a transparent semisolid was formed. The mixture was cooled to room temperature and 0.21 g methacrylic anhydride (MA) was injected as the functionalizing agent. The reaction of hydroxyl of HEMA with anhydride of MA proceeded spontaneously without using a catalyst at room temperature. The solution is stirred for 12 hours to carry out the functionalization reaction wherein reactive methacryl groups are introduced into the polymer backbone. Upon completion of the functionalization reaction, volatile acetone and residual impurities were removed by evaporation or vacuum distillation to yield a semisolid polymer precursor mixture comprising PEG 400 and methacrylate-functionalized pHEMA-co-MAA copolymer. [136] In this embodiment, the concentration of acetone in the reaction mixture may range from 10% to 80% by weight. When the acetone concentration exceeded 80% by weight, the pHEMA-co-MAA copolymer precipitated during the polymerization. When the acetone concentration was less than 10% by weight, significant gelation was caused. Gelation was caused by crosslinking of the copolymer with small amounts of divalent monomers present in HEMA as impurities. In order to obtain precursor mixtures of desired properties, it is essential to optimize the type of solvent, solvent concentration, reaction time, reaction temperature and concentration as diluent. [137] The degree of functionalization can be easily changed by adjusting the amount of MAA added to the reaction mixture as the functionalizing agent. While keeping the amounts of HEMA and MAA unchanged, various pHEMA-co-MAA copolymers of 0.3 to 5% functionality could also be synthesized according to the method described above by adjusting the amount of MA. Suitable substituents, other types of reactive groups (eg acrylates, (meth) acrylates, etc.) can be introduced into the backbone of pHEMA-co-MAA. [138] The precursor mixture obtained in this example included functionalized pHEMA-co-MAA as the prepolymer and PEG 400 as the non-reactive diluent, where the prepolymer concentration was approximately 50% by weight. This precursor mixture is further mixed with additional prepolymers such as the functionalized pHEMA obtained in Example 1, dead polymers such as pHEMA, initiators and additional non-reactive diluents to give a preferred semisolid precursor mixture which can be used directly for molding and curing. Got it. These additional components may also be introduced into the reaction medium prior to removing volatile solvents and residual impurities. [139] Example 4 pHEMA Functionalization A general method for preparing ophthalmic moldings from a pHEMA mixture. [140] Semi-solid materials for making contact lenses were prepared from functionalized pHEMA as a prepolymer, pHEMA as a dead polymer, and an unreactive diluent that is miscible with pHEMA (ie, the diluent solvates pHEMA and forms a clear mixture). [141] As an example, 0.06 g of diluent and 0.002 g of 1-hydroxycyclohexyl phenyl ketone (Irgacure 184) are added to 0.02 g of pHEMA and 0.08 g of 1% functionalized pHEMA in a vial with lid and the material is added to the oven. It was left to stand at 70 degreeC for 1 day. Typical diluents may include water, methanol, ethanol, isopropanol, propylene glycol, glycerol and PEG (300, 400, ... 1000, etc.) or mixtures thereof. In this example, a 50:50 weight mixture of ethanol and glycol was used. [142] After 1 day at 70 ° C., the resulting material was clear and relatively homogeneous semisolid. A 0.08 g weight of solvated material was hand mixed between the two glass plates for about two minutes and then placed between two ophthalmic lens molds. The assembly was placed in a 50 ° C. press and brought into contact with the mold's periphery at low pressure (this method was similar to the electrostatic casting technique commonly used in the contact lens industry). Excess semi-solid material was squeezed out of the two molds together and the amount overflowed was measured by the amount of material originally placed in the mold and the mold cavity volume. [143] Once the molds were held together, the ophthalmic moldings were cured for approximately 20 seconds under Fusion light using D-, H-, or V-bulbs. Optimizing the choice of photoinitiator and UV light source wavelengths allows for shorter curing times, with 20 seconds being the upper limit of the time required to cure this particular composition and form. The spilled material was removed by trimming the edges of the lens mold by transferring the mold assembly from the UV lamp. After cooling to room temperature, the lens mold was opened and the molding was taken out to obtain an ophthalmic lens molding. [144] The ophthalmic lens of this example included an equilibrium water content of approximately 36-38% water, depending on the degree of functionality of the starting prepolymer. The sample functionalized at about 0.5-1% exhibited a mechanical modulus similar to that observed for commercially available contact lens materials of similar water content, but could be stretched 2-4 times its original length prior to breakage. . [145] In order to produce contact lenses, the molding and curing operations of this example were also applied to precursor mixtures comprising functionalized pHEMA-co-MAA prepolymers. Since incorporation of the MAA monomer into pHEMA increases the solubility of the polymer in water, the final contact is replaced by replacing the pHEMA used in this example with, for example, the functionalized pHEMA-co-MAA prepolymer obtained in Examples 2 or 3. The equilibrium water content of the lens could be raised. The functionalized pHEMA-co-MAA prepolymers obtained in Examples 2 and 3 yielded contact lenses having an equilibrium water content of approximately 55-60% by weight. [146] In this example, the amount of non-reactive diluent may be adjusted to provide an equivalent skin exchange with water or saline solution after molding. In such cases, the cured lens had no or slight change in volume when equilibrated with water or saline solution. [147] Example 5: Moldings from 1% Functionalized pHEMA and Ophthalmic Viscosifiers [148] This example illustrates the preparation of a semisolid precursor mixture comprising a functionalized pHEMA prepolymer using various ophthalmic tackifiers as non-reactive diluents. Curing this semisolid precursor mixture formed an optically clear molding. [149] A mixture of 50% by weight of functionalized pHEMA (1% methacrylate functionality, Example 1), 25% by weight of 1,2-propylene glycol (PPG) and 25% by weight of water in a vial with a lid at 70 ° C. oven Homogenized for 1 hour, at which time the sample naturally became semisolid. This sample also contained 1% by weight of photoinitiator 4,4'-azobis (4-cyanovaleric acid) (ACVA) (based on prepolymer and diluent). This semisolid material was taken out of the oven and mixed by hand using two glass plates for several minutes. Finally the semisolid precursor mixture was pressed between two glass plates to a thickness of approximately 100 microns and then cured by placing under a diffuse UV light source (Black-Ray 700AP, UVP Inc.) for 20 minutes. Note that even using a stronger UV light source could not significantly reduce the sample cure time. [150] The molded product prepared at the time of curing was taken out of the mold and hydrated with water. The equilibrium water content was measured at approximately 39% and the sample had an elongation at break of approximately 200%. This sample was designated as number 3a in Table 1 below. [151] Other semisolid precursor mixtures were processed similarly, the formulations and results are listed in the table below (note that all samples were processed by 1% ACVA): [152] Sample No.PrepolymerdiluentWater contentElongation 3a50% pHEMA (1%)25% PPG, 25% Water39%200% 3b40% pHEMA (1%)30% PEG (400), 30% Water(Nonmeasured)(nm) 3c60% pHEMA (1%)30% PPG, 10% Water35%250% 3d60% pHEMA (1%)30% water, 10% PPG(nm)(nm) 3e48% pHEMA (1%) 12% pHEMA (5%)30% PPG, 10% Water38%200% 3f30% pHEMA (1%) 30% pHEMA (5%)30% PPG, 10% Water36%100% [153] In this example, non-functionalized pHEMA could also be added to the precursor mixture as a dead polymer without compromising optical clarity. The non-reactive diluents mentioned in this example can also be used to prepare semisolid precursor mixtures comprising functionalized pHEMA-co-MAA prepolymers comprising approximately 2% MAA. [154] Example 6: Moldings from Dead Polymers, Reactive Plasticizers, and Chemically Non-Reactive Diluents [155] This example discloses a semisolid precursor mixture comprising several dead polymers. Although the polymers were not functionalized with reactive groups, they could be functionalized via functional groups on the polymer backbone, such as hydroxyl and carboxyl groups, to obtain functionalized prepolymers. [156] A mixture comprising at least one dead polymer in a lidded vial, at least one reactive plasticizer, a photoinitiator and in certain cases an unreactive diluent, was homogenized in a 70 ° C. oven for 1 hour, at which time the sample naturally became semisolid. This semisolid material was taken out of the oven and mixed by hand using two glass plates for several minutes. Finally, the semisolid precursor mixture was pressed to a thickness of approximately 100-500 microns between the two glass plates and then cured by placing under a diffuse UV light source (Black-Ray 100AP, Uvepies Inc.) for 10-20 minutes. Note that even using a stronger UV light source could not significantly reduce the sample cure time. [157] The moldings produced upon curing were transparent, gel-like and suitable for biomedical use. Example formulations are listed in Table 2 below (all percentages were by weight): [158] Sample No.Dead polymerReactive plasticizer (s)Thinner (s)InitiatorMolding Results 4a33% polyacrylic acid33% PEG-Diacrylate33% Ethylene Glycol0.5% Irgacure 1173Transparency 4b50% pHEMA25% PEG-Diacrylate25% Ethylene Glycol0.5% Irgacure 1173Transparency 4c50% polymethyl vinyl ether-co-maleic acid25% PEG-Diacrylate25% Ethylene Glycol0.5% Irgacure 1173Transparency 4d33% Carboxy Methyl Cellulose16% PEG-Diacrylate, 16% Polybutadiene Diacrylate33% methanol0.5% Irgacure 1173Transparency 4e33% hydroxypropyl methyl cellulose16% PEG-Diacrylate, 16% Polybutadiene Diacrylate33% methanol0.5% Irgacure 1173Transparency 4f29% poly (4-vinyl pyridine)25% acrylamide, 8% methacrylated glucose48% Ethylene Glycol0.3% Irgacure 819Transparency 4 g33% Agarose17% acrylamide, 6% methacrylated glucose44% Ethylene Glycol0.3% Irgacure 819Transparency 4h50% Carboxymethyl Cellulose13% acrylamide, 4% methacrylated glucose33% Ethylene Glycol0.3% Irgacure 819Transparency 4i31% pHEMA2% tetraethylene glycol dimethacrylate67% ethanol0.5% Darcour 1173Transparency 4j53% pHEMA14% trimethylolpropane trimethacrylate33% Ethylene Glycol0.5% Irgacure 819Transparency [159] Example 7 Contact Lenses Based on a Phase Separation Iso-Refractometer [160] As an example of a phase separation isoindex system, a semisolid precursor mixture was prepared from hydrophobic silicone containing prepolymers and hydrophilic dead polymers. Functional silicone containing polymers, such as functional polydimethyl siloxane (PDMS), are commercially available with various functional groups, including (meth) acrylate functional groups that can be cured quickly by UV light. Silicone-containing polymers exhibit high oxygen permeability and have been advantageously used as the material physics for making contact lenses. [161] In this example, the prepolymer is a methacrylate functional group PDMS, where the end group of the PDMS is functionalized with a methacrylate group. The dead polymer was a HEMA based copolymer, such as a pHEMA-co-MAA based copolymer where HEMA is a major component of the copolymer. HEMA based copolymers were also functionalized with reactive groups to obtain prepolymers. Because PDMS and pHEMA are immiscible and pHEMA is more hydrophilic than PDMS, when contact lenses comprising PDMS and pHEMA based copolymers are equilibrated with water, the water is coexisting hydrophobic and hydrophilic, rich in PDMS and HEMA based copolymers, respectively. The phases were partitioned and the hydrophilic phase predominantly solvated. The refractive index of the hydrated hydrophilic phase depends on the HEMA based copolymer refractive index and the water content, which was mainly determined by the components of the copolymer. [162] The refractive indices of the pHEMA and methacrylate functional group PDMS were approximately 1.51 and 1.46, respectively. The refractive index of the pHEMA contact lens was approximately 1.44 when equilibrated with water. Thus, by molding and curing and subsequent equilibration with water, an optically transparent hydration lens was obtained, which was in the form of a phase-separated isorefractive index molding, and the refractive index of the hydrophilic phase rich in the hydrated HEMA based copolymer was consistent with that of the PDMS-rich hydrophobic phase. This was made possible by adjusting the components of the HEMA based copolymer so as to. [163] Example 8 Contact Lenses of High Oxygen Permeability and Tissue Compatibility [164] In this example, a circular disc-shaped preform was prepared from a semisolid precursor mixture, comprising a methacrylate functional group PDMS as a prepolymer, a HEMA based copolymer as a dead polymer, and a non-reactive diluent, which was prepared in Example 7 Phase separation of the refractive index mixture may be. This prepolymer was immersed in a solution of the surface forming monomer composition to impart tissue compatibility. Monomer compositions comprising HEMA and / or polyethylene glycol dimethacrylate could be used as surface forming compositions for imparting tissue compatibility. The semisolid gradient composite material formed was molded and cured into a lens by the method described in Example 4. [165] Example 9: Drug Delivery Implants with Tissue Compatibility [166] Slow or controlled release drug delivery implants were prepared from prepolymers obtained by functionalizing polysaccharides such as cellulose derivatives, chitosan and dextran. These polysaccharides could be functionalized via the hydroxyl, carboxyl and / or amine groups of the polymer backbone. Desired drugs have been included by several methods known in the art of drug delivery in semisolid precursor mixtures including functionalized polysaccharides, dead polymers, non-reactive diluents and initiators as prepolymers. The semisolid precursor mixture formed was free of potentially harmful monomer reactants that could remain as a residue upon curing. The precursor mixture was formed into a preform. [167] The preform was immersed in a solution of the surface forming composition to impart histocompatibility to obtain a gradient composite material comprising the drug. The formed preform was molded and cured to obtain a final molding that could be used as a drug delivery implant with tissue compatibility. [168] Example 10 Drug Release Contact Lenses [169] Contact lenses that act as drug delivery systems were prepared from semisolid precursor mixtures containing prepolymers, drug containing nanospheres or microspheres, and non-reactive diluents. Various methods of incorporating the drug in nanospheres or microspheres are known. Nanosphere or microsphere surface could be modified with reactive groups. When the precursor mixture included drug-containing microspheres, it was possible to advantageously form a phase separated iso-refractive system to improve optical clarity. [170] Example 11: Temperature Sensitive Drug Release Contact Lenses [171] Reusable drug release contact lenses were prepared from a semisolid precursor mixture comprising a prepolymer, a dead polymer and a non-reactive diluent. The precursor mixture could be a homogeneous mixture or a phase separated iso-refractive system. Prepolymers were prepared from polymers exhibiting solubility in temperature sensitive physiologically acceptable aqueous solutions. In order to enhance the solubility of the drug in the contact lens, the dead polymer could be selected from those showing affinity for the drug. [172] In this example, the prepolymer was based on a copolymer with N-isopropyl acrylamide as the main component, which exhibited LCST characteristics in aqueous solution. When no contact lens is used, the lens is immersed in the drug-containing solution at a lowered temperature at which the contact lens expands more than at ambient temperature, which is an efficient way of including the drug in the contact lens. When worn on the eye, the lens will release the medication slowly or in a controlled manner.
权利要求:
Claims (29) [1" claim-type="Currently amended] (i) a polymer blend consisting of at least two different prepolymers or at least one prepolymer and a dead polymer, (ii) at least one non-reactive diluent; (iii) optionally at least one reactive plasticizer; And (iv) optionally at least one active ingredient; A polymer precursor mixture, which is a semisolid polymerizable composition that exhibits low shrinkage upon polymerization. [2" claim-type="Currently amended] The polymer precursor mixture of claim 1 which is maintained optically transparent upon polymerization. [3" claim-type="Currently amended] 3. The polymer precursor mixture of claim 1 or 2 wherein the polymer precursor mixture is a semisolid water insoluble but water expandable polymerizable hydrophilic composition. [4" claim-type="Currently amended] The polymer precursor mixture according to claim 1 or 2, wherein the polymer precursor mixture forms a phase-separated iso-refractive system upon polymerization and equilibration in saline solution. [5" claim-type="Currently amended] 5. The method according to any one of claims 1 to 4, wherein the amount of said inert diluent is selected such that after the molding and curing, an exchange of blood with saline solution is provided, and the polymerized polymer precursor mixture is added to the saline solution. A polymer precursor mixture that remains optically clear upon equilibration. [6" claim-type="Currently amended] The polymer precursor mixture according to any one of claims 1 to 5, wherein the compositions of the prepolymer and the dead polymer are equal. [7" claim-type="Currently amended] The polymer precursor mixture according to claim 1, wherein the non-reactive diluent is selected from the group consisting of water, ophthalmic viscous agents and mixtures thereof. [8" claim-type="Currently amended] 8. The polymer precursor mixture according to claim 1, wherein at least one of said prepolymer and said dead polymer comprises a plurality of 2-hydroxyethyl methacrylate monomer units. 9. [9" claim-type="Currently amended] 8. The polymer precursor mixture according to claim 1, wherein at least one of the prepolymer and the dead polymer comprises a plurality of N-vinylpyrrolidone monomer units. 9. [10" claim-type="Currently amended] The polymer precursor mixture of claim 1 wherein at least one of the prepolymer and the dead polymer comprises silicone. [11" claim-type="Currently amended] The polymer precursor mixture according to any one of claims 1 to 7, wherein at least one of the prepolymer and the dead polymer is hydrophilic silicone. [12" claim-type="Currently amended] The polymer precursor mixture according to any one of claims 1 to 7, wherein at least one of the prepolymer and the dead polymer exhibits phase separation in a physiologically acceptable aqueous solution when the thermodynamic balance of the solution is shifted. [13" claim-type="Currently amended] A surface forming material and an inner core material, wherein the core material is a polymer precursor mixture according to any one of claims 1 to 12 and the composition of the surface forming material is distinct from the composition of the core forming material, the surface And the preform forming the integral whole upon polymerization. [14" claim-type="Currently amended] The preform of claim 13, wherein the surface forming material is selected from the group consisting of dye solutions, pigment solutions, scratch resistant precursor blends, hydrophilic monomer / crosslinker mixtures and mixtures thereof. [15" claim-type="Currently amended] Moldings prepared from the polymer precursor mixtures or preforms according to claim 1. [16" claim-type="Currently amended] 16. The molding according to claim 15, which exhibits minimal expansion or contraction upon equilibration in a physiologically acceptable saline solution. [17" claim-type="Currently amended] 17. The molding according to claim 15 or 16, which does not require a separate extraction step prior to the intended use. [18" claim-type="Currently amended] 18. The molding according to any one of claims 15 to 17, which is a contact lens or an intraocular lens. [19" claim-type="Currently amended] a) an initiator and (i) a polymer blend consisting of at least two different prepolymers or at least one prepolymer and a dead polymer; (ii) at least one non-reactive diluent; (iii) optionally at least one reactive plasticizer; And (iv) mixing the polymer precursor mixture, optionally comprising at least one active ingredient, together to form a semisolid polymerizable composition exhibiting low shrinkage upon polymerization; b) optionally molding the semisolid polymerizable composition into a preform of the desired form; c) optionally exposing the preform to a surface forming material to form a semisolid gradient composite material; d) introducing a semisolid polymerizable composition or semisolid gradient composite material into a mold of the desired shape; e) compacting the mold so that the semisolid polymerizable composition or semisolid gradient composite material takes the form of a cavity inside the mold; f) exposing the semisolid polymerizable composition or semisolid gradient composite material to a polymerization energy source to form a cured molding. [20" claim-type="Currently amended] 20. The method of claim 19, wherein said semisolid polymerizable composition maintains an optically clear state upon polymerization. [21" claim-type="Currently amended] 21. The method of claim 20, wherein the cured molding is a molded optical lens. [22" claim-type="Currently amended] 22. The method of any one of claims 19 to 21, wherein the polymer precursor mixture is a semisolid water insoluble but water expandable polymerizable hydrophilic composition. [23" claim-type="Currently amended] 23. The method of any of claims 19 to 22, wherein the composition of the crosslinkable prepolymer and the dead polymer are equivalent. [24" claim-type="Currently amended] 24. The method of any one of claims 19 to 23, further comprising the step of having a waiting time at a predetermined temperature after compacting said semisolid composition or said gradient composite material in a mold and prior to exposure to a source of polymerization energy. How to include. [25" claim-type="Currently amended] 25. The method of claim 19, wherein the surface forming material is applied to a mold surface, the surface forming material is optionally cured or partially cured, the preform is placed in a mold and upon mold closure. Exposing the preform to the surface forming material. [26" claim-type="Currently amended] 26. The method of any one of claims 19 to 25, further comprising placing the cured molding in a package comprising a saline solution. [27" claim-type="Currently amended] 27. The method of any of claims 19 to 26, wherein the mold can be reused. [28" claim-type="Currently amended] 28. The method of any one of claims 19 to 27, wherein the semisolid composition or the gradient composite material is exposed to a polymerization energy source for a short cure time. [29" claim-type="Currently amended] 29. The method of any of claims 19 to 28, wherein the cured molding requires only minimal extraction steps prior to its intended use.
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同族专利:
公开号 | 公开日 CN1537239A|2004-10-13| JP2004535598A|2004-11-25| TWI230165B|2005-04-01| KR100789082B1|2007-12-26| CA2451113A1|2003-01-09| BR0211041A|2004-07-20| WO2003003073A1|2003-01-09| US20030020870A1|2003-01-30| EP1407297A1|2004-04-14|
引用文献:
公开号 | 申请日 | 公开日 | 申请人 | 专利标题
法律状态:
2001-06-27|Priority to US09/894,861 2001-06-27|Priority to US09/894,861 2002-02-25|Priority to US10/083,300 2002-02-25|Priority to US10/083,300 2002-06-26|Application filed by 지엠에스, 엘엘씨 2002-06-26|Priority to PCT/US2002/022155 2004-02-18|Publication of KR20040015297A 2007-12-26|Application granted 2007-12-26|Publication of KR100789082B1
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申请号 | 申请日 | 专利标题 US09/894,861|2001-06-27| US09/894,861|US20020045706A1|1998-09-22|2001-06-27|Biomedical molding materials from semi-solid precursors| US10/083,300|US20030020870A1|2001-06-27|2002-02-25|Biomedical molding materials from semi-solid precursors| US10/083,300|2002-02-25| PCT/US2002/022155|WO2003003073A1|2001-06-27|2002-06-26|Biomedical molding materials from semi-solid precursors| 相关专利
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