 Shielded optical probe and method
专利摘要:
An optical probe, which is particularly suited to for use in measurements on tissue material of a patient. In one embodiment, the probe comprises upper and lower housing elements incorporating a light energy source and corresponding detector. The tissue material of the patient is disposed between the upper and lower housing elements such that the light energy emitted by the source passes through the tissue material to the detector. A plurality of light shields are attached to one or both of the housing elements to reduce the amount of ambient and reflected light reaching the detector. Additionally, various portions of the upper and lower housing elements and shields utilize light absorbent coloration and/or coatings which further mitigate the effects of undesired ambient and reflected light, thereby reducing noise generated within the instrument and increasing its accuracy. In one embodiment, the light shields are made removable from the optical probe, thereby facilitating replacement. A circuit for monitoring the condition of the probe, and indicating when replacement of the probe is desirable, is also disclosed. 公开号:US20010009265A1 申请号:US09/798,764 申请日:2001-03-02 公开日:2001-07-26 发明作者:Christian Schulz;Eugene Mason;Ammar Ali 申请人:Schulz Christian E.;Mason Eugene E.;Ali Ammar Al; IPC主号:A61B5-6826
专利说明:
[0001] 1. Field of the Invention [0001] [0002] The present invention relates to low-noise optical probes which may be used to sense optical energy passed through or reflected from a medium to determine the characteristics of the medium. [0002] [0003] 2. Description of the Related Art [0003] [0004] The physical characteristics of a given medium may often be determined by transmitting electromagnetic or acoustic energy through, or reflected energy from, portions of the medium. For example, in the context of medical diagnosis, light or sound energy may be directed onto a portion of a patient's body, and the fraction of that energy transmitted through (or reflected by) the patient's body measured to determine information about the various physical attributes of the patient. This type of non-invasive measurement is both more comfortable for and less deleterious to the patient than invasive techniques, and can generally be performed more quickly. [0004] [0005] Non-invasive physiological monitoring of bodily function is often required. For example, during surgery, blood oxygen saturation (oximetry) is often continuously monitored. Measurements such as these are often performed with non-invasive techniques where assessments are made by measuring the ratio of incident to transmitted (or reflected) light through an accessible part of the body such as a finger or an earlobe. A typical transmissive non-invasive monitoring device includes a light source such as a light-emitting diode (LED) placed on one side of the body part, while a photodetector is placed on an opposite side of the body part. Light energy generated by the LED is transmitted through the tissue, blood, and other portions of the body part, and detected by the photodetector on the other side. Alternatively, in a reflective device, the detector is placed on the same side of the body part as the light source, and the amount of light energy reflected by the body part measured. [0005] [0006] The transmission of optical energy passing through the body is strongly dependent on the thickness of the material through which the light passes (the optical path length). Many portions of a patient's body are typically soft and compressible. For example, a finger comprises a number of components including skin, muscle, tissue, bone, and blood. Although the bone is relatively incompressible, the tissue, muscle, and skin are easily compressible or deformed with pressure applied to the finger, as often occurs when the finger is bent. Thus, if optical energy is made incident on a patient's finger, and the patient moves in a manner which distorts or compresses the finger, the optical properties, including optical path length, may change. Since a patient generally moves in an erratic fashion, the compression of the finger is erratic and unpredictable. This causes the change in optical path length to be erratic, making the absorption of incident light energy erratic, and resulting in a measured signal which can be difficult to interpret. Similarly, movement of the patient during a reflective measurement can dramatically affect the quality of the signal obtained therefrom. [0006] [0007] In addition to the typical problem of patient movement, the presence of unwanted ambient and/or reflected light energy interferes with the measurement of the intensity of the light transmitted through or reflected by the body part. Optical transmission/reflection systems as described above utilize a light energy detector which measures, inter alia, the intensity of light transmitted to or reflected from the body part being analyzed. Since ambient light incident on the detector affects the intensity measurement, noise or error is introduced into the measured signal by such ambient light. Similarly, light generated by the light source within the measuring device (typically, an LED) which is not transmitted through or reflected by the body part under examination will also result in signal error if such light is received by the detector. These “secondary” reflections arise when light emitted by the light source is reflected by structures within the optical probe onto the detector. Accordingly, to increase the accuracy of the measurement process, both ambient light and “secondary” reflections from the light source should be mitigated. [0007] [0008] FIG. 1[0008] a illustrates an ideal signal waveform obtained from an optical probe system. FIG. 1b illustrates an actual spectra obtained from a typical optical probes not corrected for the effects of patient motion or ambient/reflected light. Note the significant increase in noise (and resulting loss of signal clarity) in FIG. 1b due to these effects. [0009] Prior optical probes have successfully addressed the issue of ease of use and patient motion during measurement. See, for example, U.S. Pat. No. 5,638,818 entitled “Low Noise Optical Probe,” assigned to the Applicant herein, which discloses a system utilizing a chamber which isolates that portion of the patient's tissue under examination from compression or movement by the patient. The device is attached to the finger of a patient, thereby readily and accurately positioning the tissue of the patient's finger over the chamber. [0009] [0010] However, attempts at limiting the effects of ambient and “secondary” reflected light have been less successful, not due to their ineffectiveness, but rather due to their obtrusiveness and relative complexity of use. A need exists, especially in the health care context, for a simple, fast, unobtrusive, and largely error-free means of non-invasive measurement of a patient's physical parameters. Especially critical is the attribute that such means be easily adapted to a variety of different patient types and characteristics with little or no adjustment, as is the device disclosed in the aforementioned patent. Prior art methods of mitigating ambient and reflected light interference have involved coverings or shrouds which substantially envelop the optical probe and tissue, thereby requiring substantial sizing and adjustment of the covering for each different patient being measured. Another disadvantage of such methods is that the placement of the patient's appendage (such as a finger) in relation to the light source and detector can not be reliably verified by the person administering the measurement unless the probe is first placed on the appendage, and the covering installed thereafter, or alternatively, unless the patient is queried. This necessitates additional time and effort on the part of the patient and the person making the measurement. [0010] [0011] Another factor relating to the efficacy of an optical probe is force distribution on the body part or tissue material being measured. Specifically, if force is distributed on the tissue material being measured unevenly or disproportionately, varying degrees of compression of the tissue may result, thereby producing a broader range of optical path lengths in the region of the light source and detector. Furthermore, if the force that the probe exerts on the tissue material is highly localized, the ability of the patient to move the tissue material with respect to the source/detector is enhanced, thereby leading to potentially increased noise levels within the signal generated by the probe. [0011] [0012] Yet another consideration relating to non-invasive optical probe measurement involves cost. In recent times, the demand has increased significantly for both disposable and reusable optical probes which are suitably constructed to provide accurate, low-noise measurements. The aforementioned prior art methods of attenuating ambient and reflected light employing coverings or shrouds carry with them a significant cost, especially if the probe (or components thereof) must be replaced on a frequent basis. Therefore, in many applications, it would be useful to have a low-cost reusable optical probe capable of attenuating ambient and reflected light, with only the degradable components being easily and cost-effectively replaced as required, without necessitating the replacement of the entire probe. Similarly, it would be useful to have a disposable probe capable of attenuating ambient and reflected light, which could be routinely replaced in its entirety a cost-effective manner. [0012] [0013] Finally, existing optical probes do not include an easy to use and reliable means for determining when to replace the probe. At present, the probe operator or health care provider must keep a record or log of the date of installation of a given probe, and replace it at a given periodicity or simply replace the probe when it seems worn out. This approach is problematic, however, not only from the standpoint of additional time and effort consumed in maintaining the record, but more significantly from the perspective that the measurement of installed time is not necessarily representative of the wear on the probe. For example, two probes installed on the same date may experience significantly different levels of wear, depending on the level of use. Alternatively, the operator could keep a log of usage, but this is too burdensome and time consuming. [0013] [0014] Based on the foregoing, a need exists for an improved low-noise optical probe which (i) is simple in design and easy to use under a variety of different operating conditions; (ii) is capable of attenuating ambient and reflected light without necessitating probe adjustment or fitting to each different patient; (iii) is capable of alerting the operator when replacement is required; and (iv) is cost effective. Such an improved probe would also ideally shield against noise caused by electromagnetic interference (EMI). [0014] SUMMARY OF THE INVENTION [0015] The present invention satisfies the foregoing needs by providing an improved optical probe for use in non-invasive energy absorption or reflection measurements, as well as a method of using the same. [0015] [0016] In a first aspect of the invention, an improved shielded optical probe assembly is disclosed which incorporates a light energy source and light energy detector embedded within a multi-part housing adapted to receive and clamp onto tissue material from the patient. When the probe is operating, light energy is directed from the light energy source through a first aperture formed within a first element of the housing and onto the tissue material of the patient, which is received within the probe. A portion of this light is transmitted through (or reflected from) the tissue material onto the detector via a second aperture. In this fashion, a light generated by the light source and transmitted through or reflected from the tissue material at a localized point is received by the detector. A light shield is fitted to the housing so as to partially surround the tissue material when it is received within the housing, thereby attenuating ambient light incident on the optical probe. In one embodiment, the light shield is made removable in order to facilitate its replacement after degradation and wear. Additionally, portions of the shield and housing are colored and/or coated such that light incident on these portions is absorbed or attenuated. The foregoing light attenuation features act to reduce the effects of noise induced within the detector (and associated processing circuitry) due to light energy not transmitted directly through or reflected from the tissue material from the light source. The probe is also optionally fitted with a diffraction grating and Faraday shield to mitigate the effects of unwanted optical modes and electromagnetic interference on probe accuracy. [0016] [0017] In a second aspect of the invention, the foregoing optical probe includes a mechanism for equalizing the force applied to the tissue of the patient when the probe is clamped thereon. In one embodiment, a series of elongated apertures each receive hinge pins which are biased apart by springs wound around the axis of the pins. When the housing elements of the probe are grasped and compressed together by the user, the hinge pins are forced against one edge of the elongated apertures, thereby providing a fulcrum for opening the probe. After the probe is opened, and the patient's finger inserted, the compressing force is removed, thereby allowing the housing elements to clamp onto the finger. As the compression force is removed, the spring bias allows the previously compressed ends of the housing elements apart, and urging the pins to the opposite edge of the elongated apertures, and “leveling” the housing elements into a more parallel orientation. This parallel orientation distributes force on the patient's finger more evenly. [0017] [0018] In a third aspect of the invention, a monitoring device is disclosed which is integrated with the optical probe circuitry in order to assist the operator in determining when to replace the probe. In one embodiment, the monitoring device is a counter which counts the number of electrical pulses generated by the detector circuitry, and correlates this number to the time of actual probe operation and percent of useful lifetime. A light emitting diode visible on the exterior of the probe is used to alert the operator to the need for probe replacement. [0018] [0019] In another aspect of the invention, a method of measuring the amount of light transmitted or reflected by the tissue material of a patient using the aforementioned optical probe is disclosed. In one embodiment of the method, the tissue material is inserted into the shielded probe housing, and light generated by the light source of the probe is transmitted via the first aperture into the tissue material. Light energy transmitted (or reflected) by the tissue material is then detected by the detector via the second aperture, and a signal relating to the intensity of the detector generated. Ambient light incident on the probe, and light generated by the light source and scattered off components other than the tissue material, are attenuated or absorbed by the shield and absorptive coating(s) during detection and signal generation in order to reduce any noise component associated therewith. The operating time of the probe is also counted in order to monitor probe remaining lifetime. [0019] BRIEF DESCRIPTION OF THE DRAWINGS [0020] FIG. 1[0020] a illustrates an ideal optical transmittance signal that would be measured by a typical prior art optical probe when utilized for blood oximetry. [0021] FIG. 1[0021] b illustrates a non-ideal optical transmittance signal measured by a typical prior art optical probe when utilized for blood oximetry. [0022] FIG. 2 is an exploded perspective view of a first embodiment of the optical probe of the present invention, configured to measure optical transmission. [0022] [0023] FIG. 2[0023] a is a perspective view of the optical probe of FIG. 2 when assembled. [0024] FIG. 2[0024] b is a perspective view of an upper support surface element of the optical probe of the present invention with a nonreflecting portion depicted with shading. [0025] FIG. 2[0025] c is a perspective view of the lower support surface element shown in FIG. 2 with a nonreflecting portion depicted with shading. [0026] FIG. 3 is a cross-sectional view of the optical probe of FIG. 2 when assembled, taken along line [0026] 3-3 thereof. [0027] FIG. 4 is a cross-sectional view of the optical probe of FIG. 2 when assembled, taken along line [0027] 4-4 thereof. [0028] FIG. 5 is a perspective view of the detector shield of the present invention, shown during assembly. [0028] [0029] FIG. 6 a perspective view of a second embodiment of the optical probe of the present invention configured to measure optical transmission. [0029] [0030] FIG. 6[0030] a is a detail plan view of the removable shield elements and channels of the optical probe of FIG. 6. [0031] FIG. 7 is a cross-sectional view of a third embodiment of the optical probe of the present invention configured to measure optical reflectance. [0031] [0032] FIG. 8 is a block diagram illustrating one embodiment of a monitoring device circuit according to the present invention. [0032] DETAILED DESCRIPTION OF THE INVENTION [0033] The invention is described in detail below with reference to the figures, wherein like elements are referenced with like numerals throughout. [0033] [0034] It is noted that the term “tissue material” as used herein includes, without limitation, the skin, tissue, blood, cartilage, ligaments, tendons, muscle, or bone of a given portion of a patient's body, such as the distal end of a finger, or any portion thereof. [0034] [0035] The term “light energy” as used herein refers to any type of electromagnetic radiation or energy, whether comprised of a narrow, discrete frequency or multiple frequencies. Examples of light energy include visible light, infrared radiation, and ultraviolet radiation. While described as an “optical” probe, the invention disclosed herein may also feasibly be used in conjunction with other forms of energy or radiation, whether optically visible or not. [0035] [0036] As shown in FIGS. 2 and 3, a first embodiment of the improved optical probe of the present invention is described. As shown in FIGS. 2 and 3, the present embodiment of the probe [0036] 100 generally comprises a two-piece housing 102, a light energy source 103, and a light energy detector 105, and an electrical supply and signal cable 107. The housing 102 consists of a first (upper) housing element 104 and a second (lower) housing element 106, which are rotatably attached to one another via a pivot element 108. The light source 103 is disposed within the upper housing element 104, while the detector is disposed within the lower housing element 106. The housing 102 of the present embodiment is adapted to receive the distal end of a finger 112 as shown in FIG. 3, with the “upper” housing element 104 engaging the upper surface 113 of the finger 112, and the “lower” housing element 106 engaging the lower surface 118 of the finger 112. It will be recognized, however, that the probe 100 may be used in any orientation, such as with the first housing element 104 being located below the second housing element 106. Furthermore, the light source 103 may alternatively be placed in the lower housing element 106, and the detector in the upper housing element 104 if desired, subject to modification of other probe components as described further below. It is also noted that while the following discussion describes a series of exemplary embodiments based on measuring the optical characteristics of a finger 112, the present invention may be adapted for use with any number of other body parts, such as earlobes or loose skin, with equal success. Hence, the specific embodiments described herein are merely illustrative of the broader invention. [0037] The first and second housing elements [0037] 104, 106 of the probe 100 of FIGS. 2 and 3 are generally rectangular in form, with the pivot element 108 being disposed near a common end 109 of each of the elongate housing elements 104, 106. The housing elements 104, 106 are in the present embodiment formed from an opaque plastic using an injection molding process of the type well known in the polymer sciences, although other materials and formation techniques may be used. The first housing element 104 includes a monitoring light emitting diode (LED) 426 visible to the operator, as is described in greater detail below with respect to FIG. 8. The first and second housing elements 104, 106 further each include support surface elements 114, 116, and one or more pairs of vertical risers 110 a-110 d with pin apertures 111 a, 111 b , the latter which are used to form the basis of the pivot element 108. The two housing elements 104, 106 are biased around the rotational axis 123 of the pivot element 108 by a biasing element, in this case a hinge spring 133 as described further below. [0038] As shown in FIG. 2, the pivot element [0038] 108 of the present embodiment comprises a hinge, and includes the aforementioned vertical risers 110 a-110 d, two hinge pins 125 a, 125 b, and biasing spring 133 located along the central axis 123 of the hinge pins 125 a, 125 b. The hinge pins 125 a, 125 b each include an outward retaining element 127, and are of a “split pin” design such that a ridge 141 located on the distal end 144 of each pin 125 engages a corresponding edge 143 of the respective interior vertical riser 110 c, 110 d of the upper housing element 104 when each pin 125 is fully received within the probe 100, as shown in FIG. 4. This arrangement, specifically the ridges 141 of the pins 125 engaging the edges 143 of their respective vertical risers 110 under an outward biasing force generated by the split in the pin, permits the pins 125 to be readily “snapped” into the apertures 111 within the vertical risers 110, thereby forming a hinge with pivot or rotational axis for the upper and lower housing elements 104, 106. The biasing spring 133 fits around the pins 125 a, 125 b as shown in FIG. 4, the two free ends 145 a, and the connecting section 1456 being received with respective holders 146 a, 146 b formed within the interior surfaces of the upper and lower housing elements 104, 106, respectively. Using this arrangement, the biasing spring 133 is preloaded (i.e., partially wound) so as to bias the upper housing element 104 against the lower housing element 106. A pair of finger recesses 150 a, 150 b are formed within the outward portion of each of the housing elements 104, 106, at a location between the common end 109 of each housing element and the pivot axis 123, thereby permitting the user to grasp the probe 100 between his or her fingers using the recesses 150 a, 150 b and separate the probe housing elements 104, 106 by applying force counter to the spring biasing force. In this fashion, the user simply grasps the probe 100, opens it by applying a light force with the grasping fingers, and inserts the distal end of the patient's finger 112 into the opened end 154 of the probe. [0039] As depicted in FIG. 2, the pin apertures [0039] 111 of the lower housing element 106 are somewhat elongated in the vertical direction (i.e., in a direction normal to the plane of the housing element 106). This feature has the practical effect of making the upper and lower housing elements 104, 106 conform more readily to the shape of the patient's finger 112 when the latter is received within the probe 100. Specifically, the elongated pin apertures allow the portion of the patient's finger 112 inserted into the open end 154 of the probe (FIG. 3) to act as a fulcrum for a “separating” force generated by the biasing springs 133 such that the common ends 109 of the upper and lower housing elements 104, 106 are forced apart by, inter alia, the bias spring separating force. This separating force is generated by the offset 160 of the bias spring ends 145 a, and connecting section 145 b from the axis 123 of the spring, as shown in FIG. 3. When the user grasps the recesses 150 of the housing elements 104, 106 and squeezes, the pins 125 are forced to the fully compressed position within the elongated pin apertures 111; that is, the pins are forced against the bottom edge of the elongated apertures 111 in order to allow the probe 100 to be opened. However, once the finger 112 is inserted into the probe, the disproportionate compression of the finger 112 (due to the interaction of the angled housing elements 104, 106 and the substantially cylindrical finger 112) and the aforementioned bias spring separating force, act to force the common end 109 of the probe housing elements 104, 106 apart, thereby making upper and lower housing elements 104, 106 more parallel to each other as shown in FIG. 3. This “dislocation” of the upper element 104 with respect to the lower element 106 allows more of the surface area of the upper and lower support surface elements 114, 116 (described below) to contact the finger 112, and for more even pressure distribution thereon. [0040] As previously discussed, the housing elements [0040] 104, 106 are adapted to receive first (upper) and second (lower) support surface elements 114, 116, respectively, which provide support and alignment for the tissue material, such as the finger 112 shown in FIG. 3, when the probe 100 is clamped thereon. When assembled as in FIGS. 2a and 3, the housing elements 104, 106 and support surface elements 114, 116 form interior cavities 115 a, 115 b within the upper and lower housing elements 104, 106, respectively, which contain, inter alia, the light source 103 and photodetector 105 as described in greater detail below. The upper support surface element 114 is fashioned from a substantially pliable polymer such as silicone rubber, so as to permit some deformation of the element 114 when in contact with the fairly rigid upper portion 113 of the patient's finger 112. In one embodiment, the upper element 114 is constructed as a membrane of polymer. The lower surface element 116 is fashioned from a substantially solid and rigid (i.e., higher durometer) polymer. This harder, solid polymer is used for the lower surface element 116 since the lower portion of the finger 112 is generally more fleshy and deformable, thereby allowing the skin and tissue material thereof to deform and contour to the shape of the inner region 122 of the lower surface element. [0041] The upper and lower surface elements [0041] 114, 116 also include first and second apertures 117, 119, respectively, which communicate with the patient's tissue material when the finger 112 is inserted in the probe 100. The apertures allow for light energy to be transmitted between the light source 103 and tissue material, and similarly between the tissue material and detector 105. The first aperture 117 is also axially located with the second aperture 119 in the vertical dimension, such that when the probe 100 is in the closed configuration with the patient's finger 112 disposed between the upper and lower surface support elements 114, 116, light emitted by the light source 103 through the first aperture 117 is transmitted through the finger 112 and the second aperture 119 and received by the detector 105. Hence, the light source 103, first aperture 117, second aperture 119, and detector 105 are substantially axial in this configuration. [0042] The lower support element [0042] 116 is further provided with a positioning element 196 disposed near the pivot element 108 and common end 109 of the probe 100, as shown in FIGS. 2 and 3. The positioning element 196 is oriented vertically with respect to the lower support element 116 so as to stop the distal end of the patient's finger from being inserted into the probe past a certain point, thereby facilitating proper alignment of the finger 112 within the probe 100, especially with respect to the source and detector apertures 117, 119. While the present embodiment uses a semi-circular tab as the positioning element 196, it will be recognized that other configurations and locations of the element 196 may be used. For example, the tab could be bifurcated with a portion being located on the upper support surface element 114, and a portion on the lower support surface element 116. Alternatively, the positioning element could be in the form of a tapered collar which receives, aligns, and restrains only the distal portion of the patient's finger. Many such alternative embodiments of the positioning element are possible, and considered to be within the scope of the present invention. [0043] As further described below, the lower surface element [0043] 116 optionally includes a chamber 126 coincident with the second aperture 119 to assist in mitigating the effects of patient movement during light transmission or reflection. The structure of such chambers is described in detail in U.S. Pat. No. 5,638,818, entitled “Low Noise Optical Probe”, which is incorporated herein by reference. In general, the chamber 126 acts to isolate a portion of the tissue material directly over the chamber 126 and aperture 119, thereby reducing compression of that tissue during movement. This tends to stabilize the signal generated by the detector 105, since the optical transmission path through the tissue material is effectively stabilized and constant. The chamber 126 is deep enough that the detector 105 and the bottom of the chamber 126 do not come into contact with the easily compressible portion of the tissue material, even when the tissue is material is caused to move. The movement of venous blood due to compression is also minimized in the field of view of the detector 105. [0044] In the embodiment of FIGS. [0044] 2-4, the light source 103 is comprised of one or more devices such as semi-conductive light emitting diodes (LEDs), although it will be appreciated that other light generating devices may be used. The light source 103 may be chosen to emit light at a single known discrete wavelength, at multiple discrete wavelengths, or across a portion of the spectrum (such as that emitted by a “white light” LED), depending on the needs of the particular application. In the present embodiment, the light source 103 consists of two diodes emitting light energy in the infrared and red regions of the electromagnetic spectrum, and a parallel resistor (or resistors) used for security. The construction and operation of such light source drive circuitry is described in U.S. Pat. No. 5,758,644 incorporated herein by reference. [0045] As shown in FIG. 2, the light source [0045] 103 is affixed in a recess 170 formed in the interior portion of the upper support surface element 114, and aligned with the aperture 117 formed within the upper support surface element 114. An adhesive such as a UV-cured silicone-based gel is used to affix the LED 103 to the recess 170, although other adhesives or attachment schemes may be employed. The light energy detector 105, in the present case a semi-conductive photodetector, is received within a corresponding recess 172 within the lower support surface element 116. As with the LED 103, the photodetector 105 may be fixed within its recess 172 according to a number of different methods, including but not limited to adhesive, a press fit, or clear epoxy resin which transmits light over a range of wavelengths of interest. [0046] As illustrated in FIG. 2, the upper support surface element [0046] 114 further includes an optical energy shield 130 which, in the present embodiment, is comprised of a plurality of shield tabs 132 a, 132 b, 132 c which protrude from the upper support surface element 114. The shield 130 and tabs 132 a, 132 b, 132 c are sized and shaped so as to conform substantially to the outer circumference of the patient's finger 112, providing at least a partial seal against ambient light incident on the probe exterior and otherwise exposed portions of the finger 112. Since the shield 130 is also formed from the same pliable polymer as the first support surface element 114, both the shield and upper support surface element are capable of automatically adapting their shape substantially to that of the patient's finger 112 without further adjustment. Specifically, as the probe 100 is closed around the finger 112, the central region of the pliable upper support surface element 114 engages the more rigid upper portion of the patient's finger, thereby compressing the element 114 in this region. This tends to draw the proximal portions 190 a, 190 b of the shield tabs 132 a, 132 b, 132 c toward the finger 112, thereby forming a better seal. In this fashion, patients having fingers of different circumferences can be accommodated with the same probe shield 130. [0047] As shown in FIGS. 2 and 3, the present embodiment of the optical probe [0047] 100 includes optional optically transparent covers 198 a, 198 b which are fitted at least partly within the apertures 117, 119 formed in the upper and lower support surface elements 114, 116, respectively. The covers 198 a, 198 b are fabricated from a rigid or semi-rigid transparent polymer (such as polycarbonate), although other materials may be substituted. The two covers 198 a, 198 b act as protection for the source 103 and detector 105 disposed thereunder, respectively. Specifically, the covers 198 are bonded to the interior surface of the upper and lower support surface elements 114, 116 such that the outer surfaces 199 a, 199 b of the covers 198 are essentially flush with the outer surfaces of their respective support surface elements 114, 116. The outer surfaces 199 a, 199 b (FIG. 3) of the covers 198 a, 198 b may also be curved or contoured if desired. It is further noted that while the present embodiment utilizes covers 198 which are optically transparent, the physical and optical properties of the covers may be adjusted to produce the desired characteristics. For example, one or both of the covers 198 a, 198 b may include a scattering medium as described further below. [0048] In an alternative embodiment, the windows for the emitter and detector are filled with a UV-cured silicone that is transparent to the wavelengths of the emitter, and the transparent covers described above are not used. [0048] [0049] In addition to the aforementioned features, the upper and lower support surface elements [0049] 114, 116 and light shield 130 are advantageously formed from or coated with a light absorbing material which further mitigates the effects of ambient light, as well as stray (i.e., “secondary”) reflected light within the probe generated by the light source 103. Specifically, light generated by the light source 103 can take several paths in reaching the detector, only one of which is the desired path via the aforementioned first and second apertures 117, 119 and through the interposed tissue material. Preferably, in order to obtain more accurate measurement of transmitted light intensity, these other paths are eliminated or attenuated. Hence, in one embodiment, the light absorbing material is disposed on the entire upper and lower surface elements 114, 116 and shield 130 so as to substantially absorb any secondary reflections prior to being received by the detector 105. In the embodiment of FIGS. 2-4, the upper surface element 114 (and integral shield 130) and lower surface element 116 may be formed from a black, opaque material which both inhibits the transmission of light energy through its thickness and absorbs at least a portion of the incident light incident onto its surface. In this fashion, the absorbing material mitigates the effects of both reflections transmitted from the light source 103, and ambient light incident on the surface elements 114, 116. It will also be appreciated that while the present embodiment employs surface elements 114, 116 which are formed from an opaque material, absorptive coatings or coverings may be used as well. For example, all or a portion of the upper and lower surface elements 114, 116 and shield 130 could be coated with a light-absorbing paint or other absorbing substance as an alternative to or in addition to the use of the aforementioned opaque material. In one embodiment, the elements 114 and 116 are white or reflective in the vicinity immediately surrounding the apertures 117, 119. [0050] For example, FIGS. 2[0050] b and 2 c depict one embodiment of the upper and lower elements 114, 116, showing nonreflective surfaces 140 a and 140 b with shading. In this embodiment, the area directly around the apertures for the LED and photodetector remain white or reflective to promote light transmission in the area of the photodetector. [0051] In addition to the light shield and absorptive materials described above, the present embodiment utilizes an electromagnetic noise shield [0051] 185 as illustrated in FIG. 5. The noise shield 185 operates on Faraday principles to block or attenuate electromagnetic interference (EMI). The noise shield 185 has a grating 187 which permits light to pass while still blocking electromagnetic energy. In a preferred embodiment, this is a very fine screen with a large open percentage to permit as much light as possible yet still block EMI. In the illustrated embodiment, the detector shield 185 is an etched copper shield made of copper foil approximately 4 mils thick, which is wrapped around the detector 105 in a box-like fashion so as to substantially enclose the detector, significantly insulating it from a external EMI. The screen or grating 187 is etched through the shield to allow light from the light source 103 to transmit through the shield 185 to the detector 105. The noise shield 185 is also electrically grounded to the detector ground, thereby precluding the buildup of electrical charge. [0052] In the optical probe of FIGS. [0052] 2-4, the apertures 117, 119 optionally may be filled wholly, or in part, by a scattering medium 180. The scattering of the light energy within a scattering medium has been found to increase the signal-to-noise ratio of the signal generated by the detector. Ideally, the scattering medium 180 scatters but does not significantly absorb light energy at the wavelengths of significance for the operation of the probe. In other words, the material is substantially transparent to optical absorption, but none-the-less effectively scatters light energy. In general, the scattering medium 180 may comprise one of a number of fixotropic substances (i.e., substances having two or more mixed materials which are conducive to scattering). The construction and use of scattering media are further described in the aforementioned U.S. Pat. No. 5,638,818. [0053] FIGS. 6 and 6[0053] a illustrate a second embodiment of the optical probe of the present invention. As illustrated, this second embodiment of the probe 200 comprises, inter alia, first and second housing elements 204, 206, upper and lower support surface elements 214, 216, and pivot assembly 208 as previously described. The embodiment of FIG. 6 further includes a plurality of discrete, removable shield tabs 220 which are mounted to the optical probe 200 using a sliding key and channel arrangement. Specifically, each of the tab elements 220 are formed such that the edge 222 which engages the optical probe 200 is shaped or keyed so as to fit within the channels 224 located on the outer portions of and running longitudinally along the upper housing element 104 of the optical probe, as shown in FIG. 6a. The present embodiment employs channels 224 and edges 222 which are substantially square in cross-section, although it will be recognized that other cross-sectional shapes including rectangles, polygons, and triangles and circles may be used with equal success. The use of a square (or other shape) for the edges 222 and their corresponding channels 224 prevents significant lateral movement or rotation of the edges 222 in the channels 224 when installed. As shown in FIG. 6a, the channels 224 may be further formed such that a pair of support ridges 225 a, 225 b act to support the tabs 220 when the latter are inserted into the channels 224, thereby adding additional rigidity to the shield tabs 220. The shield tabs 220 may also be made interchangeable from side to side if desired. [0054] The shield tabs [0054] 220 of the embodiment of FIGS. 6 and 6a are fabricated from a somewhat rigid yet flexible polymer such as silicone rubber of durometer 45A. This construction permits their removal from and insertion into the channels 224 of the housing element 204, while allowing some degree of flexibility so as to adapt to the shape and size of each individual patient's finger when the probe is fitted on the patient. [0055] It will be appreciated that while the shield tabs [0055] 220 of the present embodiment are mounted using channels disposed along the outer portions of the upper housing element 204, other locations and mounting configurations may be used. For example, the channels 224 could alternatively be located in the lower housing element 206, with the shield tabs 220 extending upward when inserted rather than downward as in FIG. 5. Similarly, the channels 224 could be located within the upper or lower support surface elements 214, 216. Furthermore, retaining mechanisms other than the aforementioned channels 224 may be used, such as pins and corresponding holes, adhesives, or other devices well known in the mechanical arts. In yet another alternative embodiment, the shield tabs 220 could be part of a single component which is received within the channels 224 or other retaining mechanism on the optical probe. A great variety of optical shield configurations according to the present invention are possible, all of which achieve the goals of minimizing noise within the probe 200 while allowing removability of the shield. [0056] As illustrated in FIG. 7, another embodiment of the optical probe of the present invention is described. In this embodiment, the probe [0056] 300 includes a light energy source 303 and detector 305, upper and lower housing elements 304, 306, upper and lower support surface elements 314, 316, and pivot element 308, as in the prior embodiment. However, the embodiment of FIG. 7 utilizes the principle of optical reflectance rather than optical transmission; hence, the light source 303 and detector 305 are both co-located within the upper housing element 304, in direct proximity to one another. Source and detector apertures 317, 319 are formed within the upper support surface element 314, their axes being canted at a predetermined angle 320 relative to the normal direction 321 and along a common plane 323. This arrangement permits light to impinge on the surface of the patient's finger 112, be reflected therefrom, and received by the detector 305 via the detector aperture 319. [0057] It will be recognized that while the source [0057] 303 and detector 305 and their respective apertures 317, 319 are located generally in the upper housing element 304 and upper support member 314, they may equally as well be located in the lower housing element 306 and support member 316 if desired. Many of such alternative orientations are possible. [0058] Additionally, although the embodiment of FIG. 7 has the axis of the apertures [0058] 317, 319 canted at a predetermined angle, such angle is not necessary for the operation of the optical probe. For example, the apertures 317, 319 could alternatively be closely co-located in a vertical orientation; light scattered from various portions of the tissue material of the patient's finger 112 beneath the source aperture 317 would be reflected into the detector aperture 319 and received by the detector 305. [0059] FIG. 8 illustrates one embodiment of the probe monitoring circuit of the present invention provided with a sensor and a monitor. In this embodiment, the monitoring circuit is comprised generally of a counter [0059] 406, non-volatile storage device 420, and monitoring LED 426. Circuitry useful for driving the light source and processing the detector signals is known in the art. The monitoring circuit counts the number of LED activations which is obtained from the modulated drive signals. For example, in one embodiment, the modulated drive pulses to at least one LEDs are also communicated to the counter 406. Specifically, the light source LEDs 103 a, 103 b are pulsed (modulated) to alternatively emit red and infrared light energy, respectively, as controlled by the LED driver 424 and the microprocessor 418. The drive signals to at least one of the LEDs also clocks the counter 406. In one preferred embodiment, the counter only increments once for a predefined number of activations. In other words, a divide by X circuit forms a portion of the counter. This is because the number of cycles is very high, and a divide circuit reduces the capacity requirements of the counter. The construction and operation of electronic counters are well known in the electrical arts, and accordingly will not be described further. Advantageously, the counter is maintained in a non-volatile RAM (NVRAM) which maintains a running count. When a predetermined number is reached, an LED 426 is activated. This number is determined by, for example, empirical data relating to the longevity of the probe to a given number of detector pulses. The monitoring LED 426 is mounted in the probe housing 102 or remotely from the probe if desired (such as on the probe control module, not shown), and is readily visible to the operator. [0060] It will be recognized that the aforementioned probe monitoring function can be accomplished using a number of different circuit configurations well known in the art. For example, in one alternative embodiment, circuitry is employed which measures the actual time the detector [0060] 105 generates an output signal. In another embodiment, the number of pulses applied to each of the LEDs 103 a, 103 b in the light source 103 is counted. Many other such alternative embodiments are possible. [0061] It will be further recognized that while the circuit of FIG. 8 utilizes an LED [0061] 426 for indicating probe age, other indicating devices such as incandescent bulbs, liquid crystal displays (LCDs), or even audio generators may be used. [0062] The pulsed emissions from the LEDs are also detected by the detector [0062] 105. The detected signals are amplified by the amplifier 402. The amplified signals are then filtered using a band-pass or other filter 404, thereby passing only that portion of the detected signals corresponding to the desired band of light intensity. [0063] The probe of the present invention may be employed in any circumstance where a measurement of transmitted or reflected energy is to be made, including but not limited to measurements taken on a finger, an earlobe, a lip, or a forehead. Thus, there are numerous other embodiments which will be obvious to one skilled in the art, including but not limited to changes in the shape of the probe and its components, changes in the materials out of which the probe is made, and changes in the shape, dimensions, and location and orientation of the apertures and shield. Furthermore, the probe of the present invention may be employed in measurements of energy or radiation other than light energy as defined herein. Depending upon the type of energy which is most advantageously utilized in a measurement, the type of transmitter or receiver of energy may be changed. The invention may be embodied in other specific forms without departing from its spirit or essential characteristics. The described embodiments are to be considered in all respects only as illustrative and not restrictive. The scope of the invention is, therefore, indicated by the appended claims rather than by the foregoing description. All changes which come within the meaning and range of equivalency of the claims are to be embraced within their scope. [0063]
权利要求:
Claims (57) [1" id="US-20010009265-A1-CLM-00001] 1. An optical probe for obtaining data from the tissue material of a living organism, comprising: an first housing element having a first support surface for supporting said tissue material, and a first aperture formed therein; a second housing element having a second support surface and a second aperture formed therein, said second housing element being located proximate to said first housing element and rotatably attached thereto so as to permit said tissue material to be positioned there between; a light source disposed within said first housing element, said light energy source being positioned such that at least a portion of the light energy emitted is transmitted through said first aperture; a light detector disposed within said second housing element, said light energy detector being positioned so as to receive at least a portion of said light energy transmitted by said light energy source through said tissue material and said second aperture; and a light shield mounted to at least one of said first and second housing elements and located proximate to said tissue material, said light shield attenuating at least a portion of ambient light energy incident on said tissue material and having a difference in attenuation properties in the area of the photodetector. [2" id="US-20010009265-A1-CLM-00002] 2. The optical probe of claim 1 , wherein said first and second housing elements are rotatably attached to one another via at least one pivot assembly. [3" id="US-20010009265-A1-CLM-00003] 3. The optical probe of claim 2 , further comprising a biasing member which biases said first and second housing elements together when said tissue material is received there between. [4" id="US-20010009265-A1-CLM-00004] 4. The optical probe of claim 3 , wherein said biasing member comprises at least one spring. [5" id="US-20010009265-A1-CLM-00005] 5. The optical probe of claim 4 , wherein said at least one spring is mounted such that its longitudinal axis is coincident with an axis of said pivot assembly. [6" id="US-20010009265-A1-CLM-00006] 6. The optical probe of claim 1 , wherein said shield comprises a plurality of shield tabs. [7" id="US-20010009265-A1-CLM-00007] 7. The optical probe of claim 6 , wherein at least one of said plurality of shield tabs is removably attached to said optical probe. [8" id="US-20010009265-A1-CLM-00008] 8. The optical probe of claim 7 , wherein said at least one of said plurality of shield tabs is attached to said optical probe using a key and channel arrangement. [9" id="US-20010009265-A1-CLM-00009] 9. The optical probe of claim 1 , wherein said shield is formed within said first support surface. [10" id="US-20010009265-A1-CLM-00010] 10. The optical probe of claim 1 , further comprising a chamber having an entrance in the form of said second aperture, wherein at least a portion of said tissue material covers said second aperture and is supported by said second support surface around said aperture, said chamber isolating at least a portion of said tissue material during optical analysis thereof. [11" id="US-20010009265-A1-CLM-00011] 11. The optical probe of claim 1 , further comprising an optical scattering medium disposed within at least one of said apertures. [12" id="US-20010009265-A1-CLM-00012] 12. The optical probe of claim 1 , further comprising a means for indicating the need for probe replacement. [13" id="US-20010009265-A1-CLM-00013] 13. The optical probe of claim 12 , wherein said means for indicating comprises a light-emitting diode, said diode being operatively coupled to a circuit capable of determining when said probe requires replacement. [14" id="US-20010009265-A1-CLM-00014] 14. An optical probe comprising: a housing capable of receiving at least a portion of the tissue material of a patient, said housing having first and second apertures formed therein, said first and second apertures being proximate to said tissue material when said tissue material is received by said housing; a light energy source disposed within said housing, said light energy source being positioned such that at least a portion of the light energy emitted thereby is transmitted through said first aperture onto said tissue material; a light energy detector disposed within said housing, said light energy detector being positioned so as to receive, via said second aperture, at least a portion of said light energy directed onto said tissue; and a light shield located proximate to said tissue material, said light shield attenuating at least a portion of ambient light energy incident on said tissue material when said tissue material is received by said housing. [15" id="US-20010009265-A1-CLM-00015] 15. The optical probe of claim 14 , wherein said housing comprises first and second housing elements, at least a portion of said tissue material being received between said first and second housing elements. [16" id="US-20010009265-A1-CLM-00016] 16. The optical probe of claim 15 , wherein said first and second housing elements are rotatably attached to one another via at least one pivot assembly. [17" id="US-20010009265-A1-CLM-00017] 17. The optical probe of claim 16 , further comprising a biasing member which biases said first and second housing elements together when said tissue material is received there between. [18" id="US-20010009265-A1-CLM-00018] 18. The optical probe of claim 17 , wherein said biasing member comprises at least one spring. [19" id="US-20010009265-A1-CLM-00019] 19. The optical probe of claim 18 , wherein said at least one spring is mounted such that its longitudinal axis is coincident with an axis of said pivot assembly. [20" id="US-20010009265-A1-CLM-00020] 20. The optical probe of claim 14 , wherein said shield comprises a plurality of shield tabs. [21" id="US-20010009265-A1-CLM-00021] 21. The optical probe of claim 20 , wherein at least one of said plurality of shield tabs is removably attached to said optical probe. [22" id="US-20010009265-A1-CLM-00022] 22. The optical probe of claim 21 , wherein said at least one of said plurality of shield tabs is attached to said optical probe using a key and channel arrangement. [23" id="US-20010009265-A1-CLM-00023] 23. The optical probe of claim 15 , further comprising first and second support surfaces for supporting said tissue material received within said optical probe, said first and second support surfaces being mounted on said first and second housing elements, respectively, and having said first and second apertures formed therein, respectively. [24" id="US-20010009265-A1-CLM-00024] 24. The optical probe of claim 23 , wherein at least a portion of said first and second support surfaces comprises an absorptive material or has an absorbtive coating capable of absorbing at least a portion of the light energy incident thereon. [25" id="US-20010009265-A1-CLM-00025] 25. The optical probe of claim 23 , wherein said shield is formed within said first support surface. [26" id="US-20010009265-A1-CLM-00026] 26. The optical probe of claim 23 , further comprising a chamber having an entrance in the form of said second aperture, wherein at least a portion of said tissue material covers said second aperture and is supported by said second support surface around said aperture, said chamber isolating at least a portion of said tissue material during optical analysis thereof. [27" id="US-20010009265-A1-CLM-00027] 27. The optical probe of claim 14 , further comprising an optical scattering medium disposed within at least one of said first and second apertures. [28" id="US-20010009265-A1-CLM-00028] 28. The optical probe of claim 14 , wherein said at least a portion of said light energy directed onto said tissue and received by said light energy detector is transmitted through at least a portion of said tissue material. [29" id="US-20010009265-A1-CLM-00029] 29. The optical probe of claim 14 , wherein said at least a portion of said light energy directed onto said tissue and received by said light energy detector is reflected from at least a portion of the surface of said tissue material. [30" id="US-20010009265-A1-CLM-00030] 30. A method of measuring a physical property using an optical probe, comprising: forming a housing element capable of receiving tissue material, said housing element having a first aperture and second aperture formed therein, said first and second apertures being located proximate to said tissue material; generating light energy using a light energy source; transmitting said light energy through said first aperture onto said tissue material; detecting, via said second aperture, at least a portion of said light energy generated by said source and transmitted onto said tissue material, using a detector; shielding said detector at least partly from light energy not generated by said light energy source and not transmitted through said first aperture; and generating a signal based on said light energy detected by said detector. [31" id="US-20010009265-A1-CLM-00031] 31. The method of claim 30 , further comprising the act of isolating at least a portion of said tissue material using a chamber formed within said housing element in order to increase the accuracy of said signal. [32" id="US-20010009265-A1-CLM-00032] 32. The method of claim 31 , further comprising the act of scattering at least a portion of said light energy generated by said optical source and an optical scattering medium disposed within at least one of said first and second apertures. [33" id="US-20010009265-A1-CLM-00033] 33. The method of claim 30 , wherein the act of shielding said detector comprises the act of absorbing at least a portion of said light energy not generated by said light energy source and not transmitted through said first aperture. [34" id="US-20010009265-A1-CLM-00034] 34. The method of claim 30 , further comprising the act of shielding said detector from electromagnetic interference using a Faraday shield. [35" id="US-20010009265-A1-CLM-00035] 35. The method of claim 30 , wherein the act of detecting at least a portion of said light energy generated by said source and transmitted onto said tissue material comprises the act of detecting light energy transmitted through said tissue material. [36" id="US-20010009265-A1-CLM-00036] 36. The method of claim 30 , wherein the act of detecting at least a portion of said light energy generated by said source and transmitted onto said tissue material comprises the act of detecting light energy reflected from the surface of said tissue material. [37" id="US-20010009265-A1-CLM-00037] 37. The method of claim 35 , further comprising the act of isolating at least a portion of said tissue material using a chamber formed within said housing element in order to increase the accuracy of said signal. [38" id="US-20010009265-A1-CLM-00038] 38. The method of claim 37 , further comprising the act of scattering at least a portion of said light energy generated by said optical source and an optical scattering medium disposed within at least one of said first and second apertures. [39" id="US-20010009265-A1-CLM-00039] 39. The method of claim 38 , wherein the act of shielding said detector comprises the act of absorbing at least a portion of said light energy not generated by said light energy source and not transmitted through said first aperture. [40" id="US-20010009265-A1-CLM-00040] 40. The method of claim 39 , further comprising the act of shielding said detector from electromagnetic interference using a Faraday shield. [41" id="US-20010009265-A1-CLM-00041] 41. The method of claim 30 , further comprising the act of counting the number of pulses detected by said detector, and comparing said number to a predetermined value. [42" id="US-20010009265-A1-CLM-00042] 42. An optical probe comprising: a housing capable of receiving at least a portion of the tissue material of a patient, said housing having first and second apertures formed therein, said first and second apertures being proximate to said tissue material when said tissue material is received by said housing, at least a portion of said housing comprising an absorptive material capable of absorbing at least a portion of the light energy incident thereon; a light energy source disposed within said housing, said light energy source being positioned such that at least a portion of the light energy emitted thereby is transmitted through said first aperture onto said tissue material; a light energy detector disposed within said housing, said light energy detector being positioned so as to receive, via said second aperture, at least a portion of said light energy transmitted onto said tissue; and a light shield located proximate to said tissue material; wherein said light shield and said absorptive material of said housing cooperate to attenuate at least a portion of any light energy both not generated by said light energy source and not transmitted through said first aperture which is incident on said tissue material when said tissue material is received by said housing. [43" id="US-20010009265-A1-CLM-00043] 43. The optical probe of claim 42 , further comprising an optical scattering medium disposed at least partly with at least one of said first and second apertures. [44" id="US-20010009265-A1-CLM-00044] 44. The optical probe of claim 42 , further comprising an electromagnetic shield used to shield said detector from electromagnetic interference. [45" id="US-20010009265-A1-CLM-00045] 45. The optical probe of claim 42 , wherein said absorptive material is a substantially black coating deposited on at least a portion of said housing element. [46" id="US-20010009265-A1-CLM-00046] 46. Data indicative of the physical condition of a patient generated using the method comprising: forming a housing element capable of receiving tissue material, said housing element having a first aperture and second aperture formed therein, said first and second apertures being located proximate to said tissue material; generating light energy using a light energy source; transmitting said light energy through said first aperture onto said tissue material; detecting, via said second aperture, at least a portion of said light energy generated by said source and transmitted onto said tissue material, using a detector; shielding said detector at least partly from light energy not generated by said light energy source and not transmitted through said first aperture; generating a signal based on said light energy detected by said detector; and analyzing said signal in order to produce said data. [47" id="US-20010009265-A1-CLM-00047] 47. The data of claim 46 , wherein the act of analyzing said signal comprises the act of processing at least a portion of said signal using a digital signal processor. [48" id="US-20010009265-A1-CLM-00048] 48. The data of claim 47 , wherein the act of processing said signal comprises performing a series of mathematical operations on said signal using said digital signal processor. [49" id="US-20010009265-A1-CLM-00049] 49. The data of claim 48 , further comprising the act of shielding said detector against electromagnetic interference using a Faraday shield. [50" id="US-20010009265-A1-CLM-00050] 50. A method of monitoring the age of an optical probe during use, comprising: generating a plurality of optical pulses; directing said plurality of optical pulses onto the tissue of a patient; detecting at least a portion of said plurality of optical pulses directed onto said tissue using a detector; generating a first signal representative of said patient's condition based on said detected optical pulses; counting the number of said portion of said plurality of optical pulses; comparing said number to a predetermined value; generating a second signal indicative of the age of said probe when said number bears a given relationship to said predetermined value. [51" id="US-20010009265-A1-CLM-00051] 51. The method of claim 50 , wherein the act of directing comprises the act of transmitting said optical pulses through at least a portion of said tissue. [52" id="US-20010009265-A1-CLM-00052] 52. The method of claim 50 , wherein the act of generating a second signal comprises the act of illuminating a light-emitting diode when said number exceeds said predetermined value. [53" id="US-20010009265-A1-CLM-00053] 53. A method of monitoring the condition of an optical probe during use by an operator, comprising: generating a plurality of optical pulses using a light energy source; detecting said plurality of optical pulses using a detector; measuring a parameter related to said optical pulses; comparing said measured parameter to a predetermined value; generating a signal indicative of said condition the when said parameter bears a given relationship to said predetermined value, said signal being perceivable by said operator. [54" id="US-20010009265-A1-CLM-00054] 54. The method of claim 53 , wherein the act of measuring a parameter related to said optical pulses comprises counting the number of optical pulses detected by said detector. [55" id="US-20010009265-A1-CLM-00055] 55. The method of claim 53 , wherein the act of measuring a parameter related to said optical pulses comprises counting the number of optical pulses generated by said light energy source. [56" id="US-20010009265-A1-CLM-00056] 56. The method of claim 53 , wherein the act of measuring a parameter related to said optical pulses comprises measuring the duration said light energy source is emitting light energy. [57" id="US-20010009265-A1-CLM-00057] 57. A system for monitoring the condition of an optical probe, comprising: at least one light source capable of generating a plurality of optical pulses; at least one photodetector capable of detecting at least a portion of said plurality of optical pulses directed onto the tissue of a patient; a monitor circuit capable of monitoring at least one parameter relating to said optical pulses, comparing said at least one parameter to a predetermined value, and generating a signal when said at least one parameter and said predetermined value are in a given relationship to each other; and an indicator, operatively connected to said monitoring circuit, said indicator generating an indication of the condition of said optical probe based on said signal.
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同族专利:
公开号 | 公开日 WO2001013790A1|2001-03-01| US6580086B1|2003-06-17| EP1206214A1|2002-05-22| JP2003507718A|2003-02-25| BR0013483A|2002-05-14| US6388240B2|2002-05-14|
引用文献:
公开号 | 申请日 | 公开日 | 申请人 | 专利标题 US20040254478A1|2003-05-22|2004-12-16|De Josselin De Jong Elbert|Fluorescence filter for tissue examination and imaging| US20050203362A1|2004-03-09|2005-09-15|Carlos Castillo|Mucosal sensor adaptor| US20070293766A1|2004-08-27|2007-12-20|Koninklijke Philips Electronics N.V.|Transmission Based Imaging for Spectroscopic Analysis| US7809420B2|2003-06-25|2010-10-05|Nellcor Puritan Bennett Llc|Hat-based oximeter sensor| US20150177222A1|2011-10-31|2015-06-25|Shenzhen Mindray Bio-Medical Electronics Co., Ltd.|Self-diagnosis method and apparatus for measuring results from blood analyzers| US20150219129A1|2013-03-12|2015-08-06|A.D. Integrity Applications Ltd.|Ear clip for medical monitoring device| WO2016143319A1|2015-03-10|2016-09-15|Nihon Kohden Corporation|Probe with inclined optical axis| US20170014076A1|2015-07-17|2017-01-19|Nihon Kohden Corporation|Probe| WO2017189660A1|2016-04-26|2017-11-02|Cote Ryan E|Electrical cables having integrated and manually controllable identification and illumination light sources| EP3434185A1|2017-07-26|2019-01-30|Koninklijke Philips N.V.|Device for measuring a physiological parameter of a human limb and method for manufacturing such device| US10506961B1|2015-04-15|2019-12-17|Eden Medical, Inc.|Diagnostic transducer and method| US10765330B2|2016-02-29|2020-09-08|Nihon Kohden Corporation|Probe for pulse photometry|US4685464A|1985-07-05|1987-08-11|Nellcor Incorporated|Durable sensor for detecting optical pulses| US4913150A|1986-08-18|1990-04-03|Physio-Control Corporation|Method and apparatus for the automatic calibration of signals employed in oximetry| JPH0217462A|1988-07-06|1990-01-22|Hitachi Ltd|Device for prevention of fault and maintenance| US5028787A|1989-01-19|1991-07-02|Futrex, Inc.|Non-invasive measurement of blood glucose| US5209230A|1990-10-19|1993-05-11|Nellcor Incorporated|Adhesive pulse oximeter sensor with reusable portion| WO1992016142A1|1991-03-21|1992-10-01|Vital Signals, Inc.|Low noise optical probe| US5313940A|1991-05-15|1994-05-24|Nihon Kohden Corporation|Photo-electric pulse wave measuring probe| US5247931A|1991-09-16|1993-09-28|Mine Safety Appliances Company|Diagnostic sensor clasp utilizing a slot, pivot and spring hinge mechanism| JPH0666633U|1993-02-26|1994-09-20|日本電気三栄株式会社|Pulse oximeter| CA2160252C|1993-04-12|2004-06-22|Robert R. Steuer|System and method for noninvasive hematocrit monitoring| JP3116259B2|1993-12-07|2000-12-11|日本光電工業株式会社|Probe for pulse oximeter| US5438986A|1993-12-14|1995-08-08|Criticare Systems, Inc.|Optical sensor| US5490523A|1994-06-29|1996-02-13|Nonin Medical Inc.|Finger clip pulse oximeter| US5851178A|1995-06-02|1998-12-22|Ohmeda Inc.|Instrumented laser diode probe connector| GB9526309D0|1995-12-22|1996-02-21|Cme Telemetrix Inc A Company O|Integrating cavity for spectroscopic measurement in light scattering samples| US5891022A|1996-09-25|1999-04-06|Ohmeda Inc.|Apparatus for performing multiwavelength photoplethysmography| JPH10314149A|1997-05-20|1998-12-02|Casio Comput Co Ltd|Probe exchangeable electric measurement device, probe management method and pulse oximeter| SE9702679D0|1997-07-11|1997-07-11|Siemens Elema Ab|Device for calculating the number of uses of a sensor| JPH1153662A|1997-07-31|1999-02-26|Aiphone Co Ltd|House information panel| JPH11185193A|1997-12-19|1999-07-09|Aiphone Co Ltd|House information panel| US5939609A|1998-03-23|1999-08-17|Conception Technology Incorporated|Multi-use sensor having a controllable number of measurement cycles|MX9702434A|1991-03-07|1998-05-31|Masimo Corp|Signal processing apparatus.| US8019400B2|1994-10-07|2011-09-13|Masimo Corporation|Signal processing apparatus| EP1905352B1|1994-10-07|2014-07-16|Masimo Corporation|Signal processing method| CA2105682C|1991-03-07|2003-09-02|Mohamed K. Diab|Signal processing apparatus and method| US5490505A|1991-03-07|1996-02-13|Masimo Corporation|Signal processing apparatus| US5638818A|1991-03-21|1997-06-17|Masimo Corporation|Low noise optical probe| US20060161071A1|1997-01-27|2006-07-20|Lynn Lawrence A|Time series objectification system and method| US9042952B2|1997-01-27|2015-05-26|Lawrence A. Lynn|System and method for automatic detection of a plurality of SPO2 time series pattern types| US9521971B2|1997-07-14|2016-12-20|Lawrence A. Lynn|System and method for automatic detection of a plurality of SPO2 time series pattern types| US6371921B1|1994-04-15|2002-04-16|Masimo Corporation|System and method of determining whether to recalibrate a blood pressure monitor| US5758644A|1995-06-07|1998-06-02|Masimo Corporation|Manual and automatic probe calibration| US6931268B1|1995-06-07|2005-08-16|Masimo Laboratories, Inc.|Active pulse blood constituent monitoring| US6027452A|1996-06-26|2000-02-22|Vital Insite, Inc.|Rapid non-invasive blood pressure measuring device| US6018673A|1996-10-10|2000-01-25|Nellcor Puritan Bennett Incorporated|Motion compatible sensor for non-invasive optical blood analysis| US9053222B2|2002-05-17|2015-06-09|Lawrence A. Lynn|Patient safety processor| US8932227B2|2000-07-28|2015-01-13|Lawrence A. Lynn|System and method for CO2 and oximetry integration| US6229856B1|1997-04-14|2001-05-08|Masimo Corporation|Method and apparatus for demodulating signals in a pulse oximetry system| US6002952A|1997-04-14|1999-12-14|Masimo Corporation|Signal processing apparatus and method| US6525386B1|1998-03-10|2003-02-25|Masimo Corporation|Non-protruding optoelectronic lens| WO1999062399A1|1998-06-03|1999-12-09|Masimo Corporation|Stereo pulse oximeter| US7245953B1|1999-04-12|2007-07-17|Masimo Corporation|Reusable pulse oximeter probe and disposable bandage apparatii| USRE41912E1|1998-10-15|2010-11-02|Masimo Corporation|Reusable pulse oximeter probe and disposable bandage apparatus| US6721585B1|1998-10-15|2004-04-13|Sensidyne, Inc.|Universal modular pulse oximeter probe for use with reusable and disposable patient attachment devices| US6463311B1|1998-12-30|2002-10-08|Masimo Corporation|Plethysmograph pulse recognition processor| US6684090B2|1999-01-07|2004-01-27|Masimo Corporation|Pulse oximetry data confidence indicator| AT434970T|2000-08-18|2009-07-15|Masimo Corp|PULSE OXIMETER WITH TWO OPERATING MODES| US20020140675A1|1999-01-25|2002-10-03|Ali Ammar Al|System and method for altering a display mode based on a gravity-responsive sensor| US6360114B1|1999-03-25|2002-03-19|Masimo Corporation|Pulse oximeter probe-off detector| US6675031B1|1999-04-14|2004-01-06|Mallinckrodt Inc.|Method and circuit for indicating quality and accuracy of physiological measurements| US6515273B2|1999-08-26|2003-02-04|Masimo Corporation|System for indicating the expiration of the useful operating life of a pulse oximetry sensor| US6676600B1|1999-09-03|2004-01-13|Tensys Medical, Inc.|Smart physiologic parameter sensor and method| US6950687B2|1999-12-09|2005-09-27|Masimo Corporation|Isolation and communication element for a resposable pulse oximetry sensor| US6377829B1|1999-12-09|2002-04-23|Masimo Corporation|Resposable pulse oximetry sensor| WO2001078593A1|2000-04-17|2001-10-25|Nellcor Puritan Bennett Incorporated|Pulse oximeter sensor with piece-wise function| US8224412B2|2000-04-17|2012-07-17|Nellcor Puritan Bennett Llc|Pulse oximeter sensor with piece-wise function| US6430525B1|2000-06-05|2002-08-06|Masimo Corporation|Variable mode averager| US6640116B2|2000-08-18|2003-10-28|Masimo Corporation|Optical spectroscopy pathlength measurement system| AU2695602A|2000-11-22|2002-06-03|Leap Wireless Int Inc|Method and system for providing interactive services over a wireless communications network| US6985764B2|2001-05-03|2006-01-10|Masimo Corporation|Flex circuit shielded optical sensor| US20060195041A1|2002-05-17|2006-08-31|Lynn Lawrence A|Centralized hospital monitoring system for automatically detecting upper airway instability and for preventing and aborting adverse drug reactions| US6850787B2|2001-06-29|2005-02-01|Masimo Laboratories, Inc.|Signal component processor| US6697658B2|2001-07-02|2004-02-24|Masimo Corporation|Low power pulse oximeter| US6754516B2|2001-07-19|2004-06-22|Nellcor Puritan Bennett Incorporated|Nuisance alarm reductions in a physiological monitor| US6748254B2|2001-10-12|2004-06-08|Nellcor Puritan Bennett Incorporated|Stacked adhesive optical sensor| US10285694B2|2001-10-20|2019-05-14|Covidien Lp|Surgical stapler with timer and feedback display| US20030212312A1|2002-01-07|2003-11-13|Coffin James P.|Low noise patient cable| US6934570B2|2002-01-08|2005-08-23|Masimo Corporation|Physiological sensor combination| US7355512B1|2002-01-24|2008-04-08|Masimo Corporation|Parallel alarm processor| US6822564B2|2002-01-24|2004-11-23|Masimo Corporation|Parallel measurement alarm processor| US7015451B2|2002-01-25|2006-03-21|Masimo Corporation|Power supply rail controller| US7317409B2|2002-01-30|2008-01-08|Tensys Medical, Inc.|Apparatus and method for interfacing time-variant signals| US6961598B2|2002-02-22|2005-11-01|Masimo Corporation|Pulse and active pulse spectraphotometry| US7509494B2|2002-03-01|2009-03-24|Masimo Corporation|Interface cable| US6850788B2|2002-03-25|2005-02-01|Masimo Corporation|Physiological measurement communications adapter| NL1021054C1|2002-07-12|2004-01-13|Best Medical Internat Beheer B|Universal measuring device for medical application.| US7096054B2|2002-08-01|2006-08-22|Masimo Corporation|Low noise optical housing| US7274955B2|2002-09-25|2007-09-25|Masimo Corporation|Parameter compensated pulse oximeter| US7142901B2|2002-09-25|2006-11-28|Masimo Corporation|Parameter compensated physiological monitor| US8412297B2|2003-10-01|2013-04-02|Covidien Lp|Forehead sensor placement| WO2004030480A1|2002-10-01|2004-04-15|Nellcor Puritan Bennett Incorporated|Headband with tension indicator| US7698909B2|2002-10-01|2010-04-20|Nellcor Puritan Bennett Llc|Headband with tension indicator| US7096052B2|2002-10-04|2006-08-22|Masimo Corporation|Optical probe including predetermined emission wavelength based on patient type| US7190986B1|2002-10-18|2007-03-13|Nellcor Puritan Bennett Inc.|Non-adhesive oximeter sensor for sensitive skin| WO2004047631A2|2002-11-22|2004-06-10|Masimo Laboratories, Inc.|Blood parameter measurement system| US6970792B1|2002-12-04|2005-11-29|Masimo Laboratories, Inc.|Systems and methods for determining blood oxygen saturation values using complex number encoding| US7006856B2|2003-01-10|2006-02-28|Nellcor Puritan Bennett Incorporated|Signal quality metrics design for qualifying data for a physiological monitor| US7016715B2|2003-01-13|2006-03-21|Nellcorpuritan Bennett Incorporated|Selection of preset filter parameters based on signal quality| US7225006B2|2003-01-23|2007-05-29|Masimo Corporation|Attachment and optical probe| US6920345B2|2003-01-24|2005-07-19|Masimo Corporation|Optical sensor including disposable and reusable elements| JP3490433B1|2003-06-02|2004-01-26|株式会社サイバーファーム|Biological information monitoring system| US20050055276A1|2003-06-26|2005-03-10|Kiani Massi E.|Sensor incentive method| US7003338B2|2003-07-08|2006-02-21|Masimo Corporation|Method and apparatus for reducing coupling between signals| US7500950B2|2003-07-25|2009-03-10|Masimo Corporation|Multipurpose sensor port| US7254431B2|2003-08-28|2007-08-07|Masimo Corporation|Physiological parameter tracking system| CN1863481A|2003-09-12|2006-11-15|福尔尼克斯医疗系统控股有限公司|Apparatus and method for medical measurement| CN101912258B|2003-10-09|2012-10-10|日本电信电话株式会社|Cuff| US7254434B2|2003-10-14|2007-08-07|Masimo Corporation|Variable pressure reusable sensor| US7483729B2|2003-11-05|2009-01-27|Masimo Corporation|Pulse oximeter access apparatus and method| US7373193B2|2003-11-07|2008-05-13|Masimo Corporation|Pulse oximetry data capture system| US7280858B2|2004-01-05|2007-10-09|Masimo Corporation|Pulse oximetry sensor| US7371981B2|2004-02-20|2008-05-13|Masimo Corporation|Connector switch| US7120479B2|2004-02-25|2006-10-10|Nellcor Puritan Bennett Inc.|Switch-mode oximeter LED drive with a single inductor| US7190985B2|2004-02-25|2007-03-13|Nellcor Puritan Bennett Inc.|Oximeter ambient light cancellation| US7438683B2|2004-03-04|2008-10-21|Masimo Corporation|Application identification sensor| US7534212B2|2004-03-08|2009-05-19|Nellcor Puritan Bennett Llc|Pulse oximeter with alternate heart-rate determination| WO2005087097A1|2004-03-08|2005-09-22|Masimo Corporation|Physiological parameter system| US7194293B2|2004-03-08|2007-03-20|Nellcor Puritan Bennett Incorporated|Selection of ensemble averaging weights for a pulse oximeter based on signal quality metrics| WO2005089640A2|2004-03-19|2005-09-29|Masimo Corporation|Low power and personal pulse oximetry systems| EP1616524A4|2004-03-29|2009-07-08|Panasonic Corp|Optical element for measuring biological information and biological information measuring instrument using it| WO2005096922A1|2004-03-31|2005-10-20|Masimo Corporation|Physiological assessment system| CA2464029A1|2004-04-08|2005-10-08|Valery Telfort|Non-invasive ventilation monitor| US9341565B2|2004-07-07|2016-05-17|Masimo Corporation|Multiple-wavelength physiological monitor| US7343186B2|2004-07-07|2008-03-11|Masimo Laboratories, Inc.|Multi-wavelength physiological monitor| US7937128B2|2004-07-09|2011-05-03|Masimo Corporation|Cyanotic infant sensor| US7254429B2|2004-08-11|2007-08-07|Glucolight Corporation|Method and apparatus for monitoring glucose levels in a biological tissue| US8036727B2|2004-08-11|2011-10-11|Glt Acquisition Corp.|Methods for noninvasively measuring analyte levels in a subject| US7976472B2|2004-09-07|2011-07-12|Masimo Corporation|Noninvasive hypovolemia monitor| WO2006039350A1|2004-09-29|2006-04-13|Masimo Corporation|Multiple key position plug| US7679519B2|2004-11-05|2010-03-16|Envitec-Wismar Gmbh|Apparatus for improved pulse oximetry measurement| US20060189871A1|2005-02-18|2006-08-24|Ammar Al-Ali|Portable patient monitor| WO2006094109A1|2005-03-01|2006-09-08|Masimo Laboratories, Inc.|Noninvasive multi-parameter patient monitor| US7392075B2|2005-03-03|2008-06-24|Nellcor Puritan Bennett Incorporated|Method for enhancing pulse oximetry calculations in the presence of correlated artifacts| CN100355390C|2005-03-15|2007-12-19|深圳迈瑞生物医疗电子股份有限公司|Method of blood oxygen probe sealing wire of silica gel finger sleeve and its mold| US7937129B2|2005-03-21|2011-05-03|Masimo Corporation|Variable aperture sensor| WO2006110859A2|2005-04-13|2006-10-19|Glucolight Corporation|Method for data reduction and calibration of an oct-based blood glucose monitor| US7464847B2|2005-06-03|2008-12-16|Tyco Healthcare Group Lp|Surgical stapler with timer and feedback display| EP3738521A1|2005-06-03|2020-11-18|Covidien LP|Surgical stapler with timer and feedback display| JP4398408B2|2005-06-16|2010-01-13|オリンパスメディカルシステムズ株式会社|Ultrasonic treatment apparatus, probe for ultrasonic treatment apparatus, and manufacturing method thereof| US7657295B2|2005-08-08|2010-02-02|Nellcor Puritan Bennett Llc|Medical sensor and technique for using the same| US7590439B2|2005-08-08|2009-09-15|Nellcor Puritan Bennett Llc|Bi-stable medical sensor and technique for using the same| US7657294B2|2005-08-08|2010-02-02|Nellcor Puritan Bennett Llc|Compliant diaphragm medical sensor and technique for using the same| US20070073116A1|2005-08-17|2007-03-29|Kiani Massi E|Patient identification using physiological sensor| US20070060808A1|2005-09-12|2007-03-15|Carine Hoarau|Medical sensor for reducing motion artifacts and technique for using the same| US8092379B2|2005-09-29|2012-01-10|Nellcor Puritan Bennett Llc|Method and system for determining when to reposition a physiological sensor| US7725147B2|2005-09-29|2010-05-25|Nellcor Puritan Bennett Llc|System and method for removing artifacts from waveforms| US7904130B2|2005-09-29|2011-03-08|Nellcor Puritan Bennett Llc|Medical sensor and technique for using the same| US7869850B2|2005-09-29|2011-01-11|Nellcor Puritan Bennett Llc|Medical sensor for reducing motion artifacts and technique for using the same| US7725146B2|2005-09-29|2010-05-25|Nellcor Puritan Bennett Llc|System and method for pre-processing waveforms| US7899510B2|2005-09-29|2011-03-01|Nellcor Puritan Bennett Llc|Medical sensor and technique for using the same| US7483731B2|2005-09-30|2009-01-27|Nellcor Puritan Bennett Llc|Medical sensor and technique for using the same| US7555327B2|2005-09-30|2009-06-30|Nellcor Puritan Bennett Llc|Folding medical sensor and technique for using the same| US7486979B2|2005-09-30|2009-02-03|Nellcor Puritan Bennett Llc|Optically aligned pulse oximetry sensor and technique for using the same| US8233954B2|2005-09-30|2012-07-31|Nellcor Puritan Bennett Llc|Mucosal sensor for the assessment of tissue and blood constituents and technique for using the same| US8062221B2|2005-09-30|2011-11-22|Nellcor Puritan Bennett Llc|Sensor for tissue gas detection and technique for using the same| US7881762B2|2005-09-30|2011-02-01|Nellcor Puritan Bennett Llc|Clip-style medical sensor and technique for using the same| US20070106126A1|2005-09-30|2007-05-10|Mannheimer Paul D|Patient monitoring alarm escalation system and method| US7962188B2|2005-10-14|2011-06-14|Masimo Corporation|Robust alarm system| US7530942B1|2005-10-18|2009-05-12|Masimo Corporation|Remote sensing infant warmer| US20070100220A1|2005-10-28|2007-05-03|Baker Clark R Jr|Adjusting parameters used in pulse oximetry analysis| US8600467B2|2006-11-29|2013-12-03|Cercacor Laboratories, Inc.|Optical sensor including disposable and reusable elements| WO2007064984A2|2005-11-29|2007-06-07|Masimo Corporation|Optical sensor including disposable and reusable elements| US7990382B2|2006-01-03|2011-08-02|Masimo Corporation|Virtual display| US8182443B1|2006-01-17|2012-05-22|Masimo Corporation|Drug administration controller| US20070191697A1|2006-02-10|2007-08-16|Lynn Lawrence A|System and method for SPO2 instability detection and quantification| US7668579B2|2006-02-10|2010-02-23|Lynn Lawrence A|System and method for the detection of physiologic response to stimulation| US20070208259A1|2006-03-06|2007-09-06|Mannheimer Paul D|Patient monitoring alarm escalation system and method| US20070244377A1|2006-03-14|2007-10-18|Cozad Jenny L|Pulse oximeter sleeve| US8219172B2|2006-03-17|2012-07-10|Glt Acquisition Corp.|System and method for creating a stable optical interface| US8702606B2|2006-03-21|2014-04-22|Covidien Lp|Patient monitoring help video system and method| US8073518B2|2006-05-02|2011-12-06|Nellcor Puritan Bennett Llc|Clip-style medical sensor and technique for using the same| US8998809B2|2006-05-15|2015-04-07|Cercacor Laboratories, Inc.|Systems and methods for calibrating minimally invasive and non-invasive physiological sensor devices| US7941199B2|2006-05-15|2011-05-10|Masimo Laboratories, Inc.|Sepsis monitor| US9176141B2|2006-05-15|2015-11-03|Cercacor Laboratories, Inc.|Physiological monitor calibration system| WO2007140478A2|2006-05-31|2007-12-06|Masimo Corporation|Respiratory monitoring| US10188348B2|2006-06-05|2019-01-29|Masimo Corporation|Parameter upgrade system| US8380271B2|2006-06-15|2013-02-19|Covidien Lp|System and method for generating customizable audible beep tones and alarms| CN100500092C|2006-06-16|2009-06-17|周常安|Blood physiological signal detecting device with changeable structure| US8145288B2|2006-08-22|2012-03-27|Nellcor Puritan Bennett Llc|Medical sensor for reducing signal artifacts and technique for using the same| US20080064965A1|2006-09-08|2008-03-13|Jay Gregory D|Devices and methods for measuring pulsus paradoxus| US8315683B2|2006-09-20|2012-11-20|Masimo Corporation|Duo connector patient cable| US8457707B2|2006-09-20|2013-06-04|Masimo Corporation|Congenital heart disease monitor| US8219170B2|2006-09-20|2012-07-10|Nellcor Puritan Bennett Llc|System and method for practicing spectrophotometry using light emitting nanostructure devices| US8175671B2|2006-09-22|2012-05-08|Nellcor Puritan Bennett Llc|Medical sensor for reducing signal artifacts and technique for using the same| US8396527B2|2006-09-22|2013-03-12|Covidien Lp|Medical sensor for reducing signal artifacts and technique for using the same| US20080103375A1|2006-09-22|2008-05-01|Kiani Massi E|Patient monitor user interface| US8190224B2|2006-09-22|2012-05-29|Nellcor Puritan Bennett Llc|Medical sensor for reducing signal artifacts and technique for using the same| US8840549B2|2006-09-22|2014-09-23|Masimo Corporation|Modular patient monitor| US9161696B2|2006-09-22|2015-10-20|Masimo Corporation|Modular patient monitor| US7869849B2|2006-09-26|2011-01-11|Nellcor Puritan Bennett Llc|Opaque, electrically nonconductive region on a medical sensor| US7574245B2|2006-09-27|2009-08-11|Nellcor Puritan Bennett Llc|Flexible medical sensor enclosure| US7796403B2|2006-09-28|2010-09-14|Nellcor Puritan Bennett Llc|Means for mechanical registration and mechanical-electrical coupling of a faraday shield to a photodetector and an electrical circuit| US7890153B2|2006-09-28|2011-02-15|Nellcor Puritan Bennett Llc|System and method for mitigating interference in pulse oximetry| US8175667B2|2006-09-29|2012-05-08|Nellcor Puritan Bennett Llc|Symmetric LED array for pulse oximetry| US8728059B2|2006-09-29|2014-05-20|Covidien Lp|System and method for assuring validity of monitoring parameter in combination with a therapeutic device| US7680522B2|2006-09-29|2010-03-16|Nellcor Puritan Bennett Llc|Method and apparatus for detecting misapplied sensors| US8068890B2|2006-09-29|2011-11-29|Nellcor Puritan Bennett Llc|Pulse oximetry sensor switchover| US8068891B2|2006-09-29|2011-11-29|Nellcor Puritan Bennett Llc|Symmetric LED array for pulse oximetry| US7684842B2|2006-09-29|2010-03-23|Nellcor Puritan Bennett Llc|System and method for preventing sensor misuse| US7476131B2|2006-09-29|2009-01-13|Nellcor Puritan Bennett Llc|Device for reducing crosstalk| US20080094228A1|2006-10-12|2008-04-24|Welch James P|Patient monitor using radio frequency identification tags| US7880626B2|2006-10-12|2011-02-01|Masimo Corporation|System and method for monitoring the life of a physiological sensor| US9192329B2|2006-10-12|2015-11-24|Masimo Corporation|Variable mode pulse indicator| JP2010506614A|2006-10-12|2010-03-04|マシモコーポレイション|Perfusion index smoothing device| US8255026B1|2006-10-12|2012-08-28|Masimo Corporation, Inc.|Patient monitor capable of monitoring the quality of attached probes and accessories| US9861305B1|2006-10-12|2018-01-09|Masimo Corporation|Method and apparatus for calibration to reduce coupling between signals in a measurement system| US8265723B1|2006-10-12|2012-09-11|Cercacor Laboratories, Inc.|Oximeter probe off indicator defining probe off space| US7772975B2|2006-10-31|2010-08-10|Corning Cable Systems, Llc|System for mapping connections using RFID function| US7782202B2|2006-10-31|2010-08-24|Corning Cable Systems, Llc|Radio frequency identification of component connections| US8414499B2|2006-12-09|2013-04-09|Masimo Corporation|Plethysmograph variability processor| US8264355B2|2006-12-14|2012-09-11|Corning Cable Systems Llc|RFID systems and methods for optical fiber network deployment and maintenance| US7760094B1|2006-12-14|2010-07-20|Corning Cable Systems Llc|RFID systems and methods for optical fiber network deployment and maintenance| US8852094B2|2006-12-22|2014-10-07|Masimo Corporation|Physiological parameter system| US7791155B2|2006-12-22|2010-09-07|Masimo Laboratories, Inc.|Detector shield| US8652060B2|2007-01-20|2014-02-18|Masimo Corporation|Perfusion trend indicator| US20080200775A1|2007-02-20|2008-08-21|Lynn Lawrence A|Maneuver-based plethysmographic pulse variation detection system and method| US20080200819A1|2007-02-20|2008-08-21|Lynn Lawrence A|Orthostasis detection system and method| US7965186B2|2007-03-09|2011-06-21|Corning Cable Systems, Llc|Passive RFID elements having visual indicators| US8280469B2|2007-03-09|2012-10-02|Nellcor Puritan Bennett Llc|Method for detection of aberrant tissue spectra| US7894869B2|2007-03-09|2011-02-22|Nellcor Puritan Bennett Llc|Multiple configuration medical sensor and technique for using the same| US8265724B2|2007-03-09|2012-09-11|Nellcor Puritan Bennett Llc|Cancellation of light shunting| US8221326B2|2007-03-09|2012-07-17|Nellcor Puritan Bennett Llc|Detection of oximetry sensor sites based on waveform characteristics| US7431188B1|2007-03-15|2008-10-07|Tyco Healthcare Group Lp|Surgical stapling apparatus with powered articulation| EP2476369B1|2007-03-27|2014-10-01|Masimo Laboratories, Inc.|Multiple wavelength optical sensor| US8800837B2|2007-04-13|2014-08-12|Covidien Lp|Powered surgical instrument| US20080255413A1|2007-04-13|2008-10-16|Michael Zemlok|Powered surgical instrument| US7950560B2|2007-04-13|2011-05-31|Tyco Healthcare Group Lp|Powered surgical instrument| US7919713B2|2007-04-16|2011-04-05|Masimo Corporation|Low noise oximetry cable including conductive cords| US8374665B2|2007-04-21|2013-02-12|Cercacor Laboratories, Inc.|Tissue profile wellness monitor| US7823760B2|2007-05-01|2010-11-02|Tyco Healthcare Group Lp|Powered surgical stapling device platform| US7931660B2|2007-05-10|2011-04-26|Tyco Healthcare Group Lp|Powered tacker instrument| US8602997B2|2007-06-12|2013-12-10|Sotera Wireless, Inc.|Body-worn system for measuring continuous non-invasive blood pressure | WO2008154643A1|2007-06-12|2008-12-18|Triage Wireless, Inc.|Vital sign monitor for measuring blood pressure using optical, electrical, and pressure waveforms| US8764671B2|2007-06-28|2014-07-01|Masimo Corporation|Disposable active pulse sensor| US8048040B2|2007-09-13|2011-11-01|Masimo Corporation|Fluid titration system| US8960520B2|2007-10-05|2015-02-24|Covidien Lp|Method and apparatus for determining parameters of linear motion in a surgical instrument| US8967443B2|2007-10-05|2015-03-03|Covidien Lp|Method and apparatus for determining parameters of linear motion in a surgical instrument| US20090090763A1|2007-10-05|2009-04-09|Tyco Healthcare Group Lp|Powered surgical stapling device| JP5296793B2|2007-10-12|2013-09-25|マシモコーポレイション|Connector assembly| USD609193S1|2007-10-12|2010-02-02|Masimo Corporation|Connector assembly| US8355766B2|2007-10-12|2013-01-15|Masimo Corporation|Ceramic emitter substrate| US8310336B2|2008-10-10|2012-11-13|Masimo Corporation|Systems and methods for storing, analyzing, retrieving and displaying streaming medical data| WO2009049254A2|2007-10-12|2009-04-16|Masimo Corporation|Systems and methods for storing, analyzing, and retrieving medical data| US7922063B2|2007-10-31|2011-04-12|Tyco Healthcare Group, Lp|Powered surgical instrument| US8204567B2|2007-12-13|2012-06-19|Nellcor Puritan Bennett Llc|Signal demodulation| US8346328B2|2007-12-21|2013-01-01|Covidien Lp|Medical sensor and technique for using the same| US8352004B2|2007-12-21|2013-01-08|Covidien Lp|Medical sensor and technique for using the same| US8366613B2|2007-12-26|2013-02-05|Covidien Lp|LED drive circuit for pulse oximetry and method for using same| US20090171167A1|2007-12-27|2009-07-02|Nellcor Puritan Bennett Llc|System And Method For Monitor Alarm Management| US8577434B2|2007-12-27|2013-11-05|Covidien Lp|Coaxial LED light sources| US8442608B2|2007-12-28|2013-05-14|Covidien Lp|System and method for estimating physiological parameters by deconvolving artifacts| US8452364B2|2007-12-28|2013-05-28|Covidien LLP|System and method for attaching a sensor to a patient's skin| US8897850B2|2007-12-31|2014-11-25|Covidien Lp|Sensor with integrated living hinge and spring| US8092993B2|2007-12-31|2012-01-10|Nellcor Puritan Bennett Llc|Hydrogel thin film for use as a biosensor| US8199007B2|2007-12-31|2012-06-12|Nellcor Puritan Bennett Llc|Flex circuit snap track for a biometric sensor| US8070508B2|2007-12-31|2011-12-06|Nellcor Puritan Bennett Llc|Method and apparatus for aligning and securing a cable strain relief| US8750953B2|2008-02-19|2014-06-10|Covidien Lp|Methods and systems for alerting practitioners to physiological conditions| US8275553B2|2008-02-19|2012-09-25|Nellcor Puritan Bennett Llc|System and method for evaluating physiological parameter data| USD614305S1|2008-02-29|2010-04-20|Masimo Corporation|Connector assembly| US8768423B2|2008-03-04|2014-07-01|Glt Acquisition Corp.|Multispot monitoring for use in optical coherence tomography| US20090247851A1|2008-03-26|2009-10-01|Nellcor Puritan Bennett Llc|Graphical User Interface For Monitor Alarm Management| US8140272B2|2008-03-27|2012-03-20|Nellcor Puritan Bennett Llc|System and method for unmixing spectroscopic observations with nonnegative matrix factorization| US8437822B2|2008-03-28|2013-05-07|Covidien Lp|System and method for estimating blood analyte concentration| US8364224B2|2008-03-31|2013-01-29|Covidien Lp|System and method for facilitating sensor and monitor communication| US8112375B2|2008-03-31|2012-02-07|Nellcor Puritan Bennett Llc|Wavelength selection and outlier detection in reduced rank linear models| US8292809B2|2008-03-31|2012-10-23|Nellcor Puritan Bennett Llc|Detecting chemical components from spectroscopic observations| US20090265226A1|2008-04-16|2009-10-22|Stephen Martiros|Methods and apparatus for interactive advertising| US20090265665A1|2008-04-16|2009-10-22|Stephen Martiros|Methods and apparatus for interactive advertising| EP2278911A1|2008-05-02|2011-02-02|Masimo Corporation|Monitor configuration system| EP2312995B1|2008-05-05|2017-06-28|Masimo Corporation|Pulse oximetry system with electrical decoupling circuitry| JP5474937B2|2008-05-07|2014-04-16|ローレンスエー. リン,|Medical disorder pattern search engine| US9895068B2|2008-06-30|2018-02-20|Covidien Lp|Pulse oximeter with wait-time indication| USD626561S1|2008-06-30|2010-11-02|Nellcor Puritan Bennett Llc|Circular satseconds indicator and triangular saturation pattern detection indicator for a patient monitor display panel| USD626562S1|2008-06-30|2010-11-02|Nellcor Puritan Bennett Llc|Triangular saturation pattern detection indicator for a patient monitor display panel| US8071935B2|2008-06-30|2011-12-06|Nellcor Puritan Bennett Llc|Optical detector with an overmolded faraday shield| US7880884B2|2008-06-30|2011-02-01|Nellcor Puritan Bennett Llc|System and method for coating and shielding electronic sensor components| US20090327515A1|2008-06-30|2009-12-31|Thomas Price|Medical Monitor With Network Connectivity| US7887345B2|2008-06-30|2011-02-15|Nellcor Puritan Bennett Llc|Single use connector for pulse oximetry sensors| WO2010003134A2|2008-07-03|2010-01-07|Masimo Laboratories, Inc.|Protrusion, heat sink, and shielding for improving spectroscopic measurement of blood constituents| US8248208B2|2008-07-15|2012-08-21|Corning Cable Systems, Llc.|RFID-based active labeling system for telecommunication systems| US8203438B2|2008-07-29|2012-06-19|Masimo Corporation|Alarm suspend system| CN102165304B|2008-07-30|2014-10-29|皮尼奥洛股份公司|Diode laser device for the non-invasive measurement of glycaemia| US20100030040A1|2008-08-04|2010-02-04|Masimo Laboratories, Inc.|Multi-stream data collection system for noninvasive measurement of blood constituents| USD621516S1|2008-08-25|2010-08-10|Masimo Laboratories, Inc.|Patient monitoring sensor| US8731405B2|2008-08-28|2014-05-20|Corning Cable Systems Llc|RFID-based systems and methods for collecting telecommunications network information| SE532941C2|2008-09-15|2010-05-18|Phasein Ab|Gas sampling line for breathing gases| US8911377B2|2008-09-15|2014-12-16|Masimo Corporation|Patient monitor including multi-parameter graphical display| US8364220B2|2008-09-25|2013-01-29|Covidien Lp|Medical sensor and technique for using the same| US8257274B2|2008-09-25|2012-09-04|Nellcor Puritan Bennett Llc|Medical sensor and technique for using the same| US8914088B2|2008-09-30|2014-12-16|Covidien Lp|Medical sensor and technique for using the same| US8433382B2|2008-09-30|2013-04-30|Covidien Lp|Transmission mode photon density wave system and method| US8386000B2|2008-09-30|2013-02-26|Covidien Lp|System and method for photon density wave pulse oximetry and pulse hemometry| US8417309B2|2008-09-30|2013-04-09|Covidien Lp|Medical sensor| US8423112B2|2008-09-30|2013-04-16|Covidien Lp|Medical sensor and technique for using the same| US8968193B2|2008-09-30|2015-03-03|Covidien Lp|System and method for enabling a research mode on physiological monitors| US8346330B2|2008-10-13|2013-01-01|Masimo Corporation|Reflection-detector sensor position indicator| US8401602B2|2008-10-13|2013-03-19|Masimo Corporation|Secondary-emitter sensor position indicator| GB2465230B|2008-11-17|2013-08-21|Dialog Devices Ltd|Assessing a subject's circulatory system| US8771204B2|2008-12-30|2014-07-08|Masimo Corporation|Acoustic sensor assembly| US8588880B2|2009-02-16|2013-11-19|Masimo Corporation|Ear sensor| US10032002B2|2009-03-04|2018-07-24|Masimo Corporation|Medical monitoring system| US9218454B2|2009-03-04|2015-12-22|Masimo Corporation|Medical monitoring system| US10007758B2|2009-03-04|2018-06-26|Masimo Corporation|Medical monitoring system| US8388353B2|2009-03-11|2013-03-05|Cercacor Laboratories, Inc.|Magnetic connector| US8452366B2|2009-03-16|2013-05-28|Covidien Lp|Medical monitoring device with flexible circuitry| US8897847B2|2009-03-23|2014-11-25|Masimo Corporation|Digit gauge for noninvasive optical sensor| US8221319B2|2009-03-25|2012-07-17|Nellcor Puritan Bennett Llc|Medical device for assessing intravascular blood volume and technique for using the same| US8515515B2|2009-03-25|2013-08-20|Covidien Lp|Medical sensor with compressible light barrier and technique for using the same| US8781548B2|2009-03-31|2014-07-15|Covidien Lp|Medical sensor with flexible components and technique for using the same| JP5428510B2|2009-05-12|2014-02-26|富士通株式会社|Pulse wave acquisition device and pulse measurement device| US8509869B2|2009-05-15|2013-08-13|Covidien Lp|Method and apparatus for detecting and analyzing variations in a physiologic parameter| JP5584997B2|2009-05-15|2014-09-10|コニカミノルタ株式会社|Probe for measuring biological information| JP5402229B2|2009-05-15|2014-01-29|コニカミノルタ株式会社|Probe for measuring biological information| US8989831B2|2009-05-19|2015-03-24|Masimo Corporation|Disposable components for reusable physiological sensor| US20100298654A1|2009-05-20|2010-11-25|Triage Wireless, Inc.|Blood pressure-monitoring system with alarm/alert system that accounts for patient motion| US8956294B2|2009-05-20|2015-02-17|Sotera Wireless, Inc.|Body-worn system for continuously monitoring a patients BP, HR, SpO2, RR, temperature, and motion; also describes specific monitors for apnea, ASY, VTAC, VFIB, and ‘bed sore’ index| US8571619B2|2009-05-20|2013-10-29|Masimo Corporation|Hemoglobin display and patient treatment| US8634891B2|2009-05-20|2014-01-21|Covidien Lp|Method and system for self regulation of sensor component contact pressure| US8821514B2|2009-06-08|2014-09-02|Covidien Lp|Powered tack applier| US8418524B2|2009-06-12|2013-04-16|Masimo Corporation|Non-invasive sensor calibration device| US9596999B2|2009-06-17|2017-03-21|Sotera Wireless, Inc.|Body-worn pulse oximeter| US8670811B2|2009-06-30|2014-03-11|Masimo Corporation|Pulse oximetry system for adjusting medical ventilation| US8505821B2|2009-06-30|2013-08-13|Covidien Lp|System and method for providing sensor quality assurance| US8311601B2|2009-06-30|2012-11-13|Nellcor Puritan Bennett Llc|Reflectance and/or transmissive pulse oximeter| US9010634B2|2009-06-30|2015-04-21|Covidien Lp|System and method for linking patient data to a patient and providing sensor quality assurance| US8391941B2|2009-07-17|2013-03-05|Covidien Lp|System and method for memory switching for multiple configuration medical sensor| US8471713B2|2009-07-24|2013-06-25|Cercacor Laboratories, Inc.|Interference detector for patient monitor| US8473020B2|2009-07-29|2013-06-25|Cercacor Laboratories, Inc.|Non-invasive physiological sensor cover| US8494786B2|2009-07-30|2013-07-23|Covidien Lp|Exponential sampling of red and infrared signals| US8417310B2|2009-08-10|2013-04-09|Covidien Lp|Digital switching in multi-site sensor| US8428675B2|2009-08-19|2013-04-23|Covidien Lp|Nanofiber adhesives used in medical devices| US8494606B2|2009-08-19|2013-07-23|Covidien Lp|Photoplethysmography with controlled application of sensor pressure| US8688183B2|2009-09-03|2014-04-01|Ceracor Laboratories, Inc.|Emitter driver for noninvasive patient monitor| US20110066043A1|2009-09-14|2011-03-17|Matt Banet|System for measuring vital signs during hemodialysis| US20110172498A1|2009-09-14|2011-07-14|Olsen Gregory A|Spot check monitor credit system| US20110066008A1|2009-09-14|2011-03-17|Matt Banet|Body-worn monitor for measuring respiration rate| US8527038B2|2009-09-15|2013-09-03|Sotera Wireless, Inc.|Body-worn vital sign monitor| US10420476B2|2009-09-15|2019-09-24|Sotera Wireless, Inc.|Body-worn vital sign monitor| US10806351B2|2009-09-15|2020-10-20|Sotera Wireless, Inc.|Body-worn vital sign monitor| US20110137297A1|2009-09-17|2011-06-09|Kiani Massi Joe E|Pharmacological management system| US9510779B2|2009-09-17|2016-12-06|Masimo Corporation|Analyte monitoring using one or more accelerometers| US8704666B2|2009-09-21|2014-04-22|Covidien Lp|Medical device interface customization systems and methods| US8788001B2|2009-09-21|2014-07-22|Covidien Lp|Time-division multiplexing in a multi-wavelength photon density wave system| US8494604B2|2009-09-21|2013-07-23|Covidien Lp|Wavelength-division multiplexing in a multi-wavelength photon density wave system| US8798704B2|2009-09-24|2014-08-05|Covidien Lp|Photoacoustic spectroscopy method and system to discern sepsis from shock| US8571618B1|2009-09-28|2013-10-29|Cercacor Laboratories, Inc.|Adaptive calibration system for spectrophotometric measurements| US8515511B2|2009-09-29|2013-08-20|Covidien Lp|Sensor with an optical coupling material to improve plethysmographic measurements and method of using the same| US8376955B2|2009-09-29|2013-02-19|Covidien Lp|Spectroscopic method and system for assessing tissue temperature| US9554739B2|2009-09-29|2017-01-31|Covidien Lp|Smart cable for coupling a medical sensor to an electronic patient monitor| US20110077470A1|2009-09-30|2011-03-31|Nellcor Puritan Bennett Llc|Patient Monitor Symmetry Control| US20110082711A1|2009-10-06|2011-04-07|Masimo Laboratories, Inc.|Personal digital assistant or organizer for monitoring glucose levels| US8523781B2|2009-10-15|2013-09-03|Masimo Corporation|Bidirectional physiological information display| US8430817B1|2009-10-15|2013-04-30|Masimo Corporation|System for determining confidence in respiratory rate measurements| US8715206B2|2009-10-15|2014-05-06|Masimo Corporation|Acoustic patient sensor| US9106038B2|2009-10-15|2015-08-11|Masimo Corporation|Pulse oximetry system with low noise cable hub| US10463340B2|2009-10-15|2019-11-05|Masimo Corporation|Acoustic respiratory monitoring systems and methods| WO2011047216A2|2009-10-15|2011-04-21|Masimo Corporation|Physiological acoustic monitoring system| US9848800B1|2009-10-16|2017-12-26|Masimo Corporation|Respiratory pause detector| US9839381B1|2009-11-24|2017-12-12|Cercacor Laboratories, Inc.|Physiological measurement system with automatic wavelength adjustment| WO2011069122A1|2009-12-04|2011-06-09|Masimo Corporation|Calibration for multi-stage physiological monitors| US9153112B1|2009-12-21|2015-10-06|Masimo Corporation|Modular patient monitor| JP2013521054A|2010-03-01|2013-06-10|マシモコーポレイション|Adaptive alarm system| EP2544591B1|2010-03-08|2021-07-21|Masimo Corporation|Reprocessing of aphysiological sensor| US10213159B2|2010-03-10|2019-02-26|Sotera Wireless, Inc.|Body-worn vital sign monitor| US9307928B1|2010-03-30|2016-04-12|Masimo Corporation|Plethysmographic respiration processor| US9386931B2|2010-03-31|2016-07-12|Covidien Lp|System and method for receiving an indication of proper body locations of sensors on a patient| US8517241B2|2010-04-16|2013-08-27|Covidien Lp|Hand-held surgical devices| US9173593B2|2010-04-19|2015-11-03|Sotera Wireless, Inc.|Body-worn monitor for measuring respiratory rate| US9339209B2|2010-04-19|2016-05-17|Sotera Wireless, Inc.|Body-worn monitor for measuring respiratory rate| US8979765B2|2010-04-19|2015-03-17|Sotera Wireless, Inc.|Body-worn monitor for measuring respiratory rate| US8747330B2|2010-04-19|2014-06-10|Sotera Wireless, Inc.|Body-worn monitor for measuring respiratory rate| US9173594B2|2010-04-19|2015-11-03|Sotera Wireless, Inc.|Body-worn monitor for measuring respiratory rate| US8888700B2|2010-04-19|2014-11-18|Sotera Wireless, Inc.|Body-worn monitor for measuring respiratory rate| US8712494B1|2010-05-03|2014-04-29|Masimo Corporation|Reflective non-invasive sensor| US9138180B1|2010-05-03|2015-09-22|Masimo Corporation|Sensor adapter cable| US8666468B1|2010-05-06|2014-03-04|Masimo Corporation|Patient monitor for determining microcirculation state| US9326712B1|2010-06-02|2016-05-03|Masimo Corporation|Opticoustic sensor| US8740792B1|2010-07-12|2014-06-03|Masimo Corporation|Patient monitor capable of accounting for environmental conditions| US9408542B1|2010-07-22|2016-08-09|Masimo Corporation|Non-invasive blood pressure measurement system| US8930145B2|2010-07-28|2015-01-06|Covidien Lp|Light focusing continuous wave photoacoustic spectroscopy and its applications to patient monitoring| WO2012027613A1|2010-08-26|2012-03-01|Masimo Corporation|Blood pressure measurement system| US8821397B2|2010-09-28|2014-09-02|Masimo Corporation|Depth of consciousness monitor including oximeter| US9775545B2|2010-09-28|2017-10-03|Masimo Corporation|Magnetic electrical connector for patient monitors| US9211095B1|2010-10-13|2015-12-15|Masimo Corporation|Physiological measurement logic engine| US8723677B1|2010-10-20|2014-05-13|Masimo Corporation|Patient safety system with automatically adjusting bed| US20120226117A1|2010-12-01|2012-09-06|Lamego Marcelo M|Handheld processing device including medical applications for minimally and non invasive glucose measurements| CN105832317B|2010-12-28|2020-02-14|索泰拉无线公司|System for measuring cardiac output, stroke volume, heart force and blood pressure| US9579039B2|2011-01-10|2017-02-28|Masimo Corporation|Non-invasive intravascular volume index monitor| WO2012109671A1|2011-02-13|2012-08-16|Masimo Corporation|Medical characterization system| WO2012112891A1|2011-02-18|2012-08-23|Sotera Wireless, Inc.|Modular wrist-worn processor for patient monitoring| SG10201601161YA|2011-02-18|2016-03-30|Sotera Wireless Inc|Optical sensor for measuring physiological properties| US9066666B2|2011-02-25|2015-06-30|Cercacor Laboratories, Inc.|Patient monitor for monitoring microcirculation| US8830449B1|2011-04-18|2014-09-09|Cercacor Laboratories, Inc.|Blood analysis system| US9095316B2|2011-04-20|2015-08-04|Masimo Corporation|System for generating alarms based on alarm patterns| US9622692B2|2011-05-16|2017-04-18|Masimo Corporation|Personal health device| US9986919B2|2011-06-21|2018-06-05|Masimo Corporation|Patient monitoring system| US9532722B2|2011-06-21|2017-01-03|Masimo Corporation|Patient monitoring system| USD668340S1|2011-06-29|2012-10-02|Beijing Choice Electronic Technology Co., Ltd.|Finger-clipped pulse oximeter| US9245668B1|2011-06-29|2016-01-26|Cercacor Laboratories, Inc.|Low noise cable providing communication between electronic sensor components and patient monitor| US9192351B1|2011-07-22|2015-11-24|Masimo Corporation|Acoustic respiratory monitoring sensor with probe-off detection| US8755872B1|2011-07-28|2014-06-17|Masimo Corporation|Patient monitoring system for indicating an abnormal condition| US9782077B2|2011-08-17|2017-10-10|Masimo Corporation|Modulated physiological sensor| US9323894B2|2011-08-19|2016-04-26|Masimo Corporation|Health care sanitation monitoring system| WO2013056160A2|2011-10-13|2013-04-18|Masimo Corporation|Medical monitoring hub| WO2013056141A1|2011-10-13|2013-04-18|Masimo Corporation|Physiological acoustic monitoring system| US9808188B1|2011-10-13|2017-11-07|Masimo Corporation|Robust fractional saturation determination| US9943269B2|2011-10-13|2018-04-17|Masimo Corporation|System for displaying medical monitoring data| US9778079B1|2011-10-27|2017-10-03|Masimo Corporation|Physiological monitor gauge panel| US20130109963A1|2011-10-31|2013-05-02|The University Of Connecticut|Method and apparatus for medical imaging using combined near-infrared optical tomography, fluorescent tomography and ultrasound| US9445759B1|2011-12-22|2016-09-20|Cercacor Laboratories, Inc.|Blood glucose calibration system| US11172890B2|2012-01-04|2021-11-16|Masimo Corporation|Automated condition screening and detection| US9392945B2|2012-01-04|2016-07-19|Masimo Corporation|Automated CCHD screening and detection| US10149616B2|2012-02-09|2018-12-11|Masimo Corporation|Wireless patient monitoring device| US10307111B2|2012-02-09|2019-06-04|Masimo Corporation|Patient position detection system| US9480435B2|2012-02-09|2016-11-01|Masimo Corporation|Configurable patient monitoring system| US9195385B2|2012-03-25|2015-11-24|Masimo Corporation|Physiological monitor touchscreen interface| US9833146B2|2012-04-17|2017-12-05|Covidien Lp|Surgical system and method of use of the same| US9131881B2|2012-04-17|2015-09-15|Masimo Corporation|Hypersaturation index| WO2013184965A1|2012-06-07|2013-12-12|Masimo Corporation|Depth of consciousness monitor| JP5627644B2|2012-06-19|2014-11-19|Jfeアドバンテック株式会社|Fluorescence detector| US9697928B2|2012-08-01|2017-07-04|Masimo Corporation|Automated assembly sensor cable| US9636025B2|2012-08-15|2017-05-02|Nanyang Technological University|Systems and methods for pedal revascularization assessment| US10827961B1|2012-08-29|2020-11-10|Masimo Corporation|Physiological measurement calibration| US9749232B2|2012-09-20|2017-08-29|Masimo Corporation|Intelligent medical network edge router| US9955937B2|2012-09-20|2018-05-01|Masimo Corporation|Acoustic patient sensor coupler| US9563832B2|2012-10-08|2017-02-07|Corning Incorporated|Excess radio-frequencypower storage and power sharing RF identificationtags, and related connection systems and methods| US9717458B2|2012-10-20|2017-08-01|Masimo Corporation|Magnetic-flap optical sensor| US9560996B2|2012-10-30|2017-02-07|Masimo Corporation|Universal medical system| US9787568B2|2012-11-05|2017-10-10|Cercacor Laboratories, Inc.|Physiological test credit method| US9750461B1|2013-01-02|2017-09-05|Masimo Corporation|Acoustic respiratory monitoring sensor with probe-off detection| US9724025B1|2013-01-16|2017-08-08|Masimo Corporation|Active-pulse blood analysis system| US11206990B2|2013-01-23|2021-12-28|Pedra Technology Pte Ltd|Deep tissue flowmetry using diffuse speckle contrast analysis| US9750442B2|2013-03-09|2017-09-05|Masimo Corporation|Physiological status monitor| US10441181B1|2013-03-13|2019-10-15|Masimo Corporation|Acoustic pulse and respiration monitoring system| US9965946B2|2013-03-13|2018-05-08|Masimo Corporation|Systems and methods for monitoring a patient health network| WO2014159132A1|2013-03-14|2014-10-02|Cercacor Laboratories, Inc.|Systems and methods for testing patient monitors| WO2014158820A1|2013-03-14|2014-10-02|Cercacor Laboratories, Inc.|Patient monitor as a minimally invasive glucometer| US9936917B2|2013-03-14|2018-04-10|Masimo Laboratories, Inc.|Patient monitor placement indicator| US9986952B2|2013-03-14|2018-06-05|Masimo Corporation|Heart sound simulator| US10456038B2|2013-03-15|2019-10-29|Cercacor Laboratories, Inc.|Cloud-based physiological monitoring system| US20140350367A1|2013-05-21|2014-11-27|GestIn Time, Inc.|Peak flow meter, breathalyzer, and pulse oximeter for use with a mobile device| US9891079B2|2013-07-17|2018-02-13|Masimo Corporation|Pulser with double-bearing position encoder for non-invasive physiological monitoring| US10555678B2|2013-08-05|2020-02-11|Masimo Corporation|Blood pressure monitor with valve-chamber assembly| EP3054849A2|2013-10-07|2016-08-17|Masimo Corporation|Regional oximetry sensor| US11147518B1|2013-10-07|2021-10-19|Masimo Corporation|Regional oximetry signal processor| US10832818B2|2013-10-11|2020-11-10|Masimo Corporation|Alarm notification system| US10828007B1|2013-10-11|2020-11-10|Masimo Corporation|Acoustic sensor with attachment portion| US10279247B2|2013-12-13|2019-05-07|Masimo Corporation|Avatar-incentive healthcare therapy| US10086138B1|2014-01-28|2018-10-02|Masimo Corporation|Autonomous drug delivery system| US10532174B2|2014-02-21|2020-01-14|Masimo Corporation|Assistive capnography device| US9924897B1|2014-06-12|2018-03-27|Masimo Corporation|Heated reprocessing of physiological sensors| US10231670B2|2014-06-19|2019-03-19|Masimo Corporation|Proximity sensor in pulse oximeter| US10231657B2|2014-09-04|2019-03-19|Masimo Corporation|Total hemoglobin screening sensor| US10383520B2|2014-09-18|2019-08-20|Masimo Semiconductor, Inc.|Enhanced visible near-infrared photodiode and non-invasive physiological sensor| WO2016057553A1|2014-10-07|2016-04-14|Masimo Corporation|Modular physiological sensors| EP3023053A1|2014-11-21|2016-05-25|Nokia Technologies OY|Apparatus and method for sensing light| WO2016118922A1|2015-01-23|2016-07-28|Masimo Sweden Ab|Nasal/oral cannula system and manufacturing| USD755392S1|2015-02-06|2016-05-03|Masimo Corporation|Pulse oximetry sensor| US10568553B2|2015-02-06|2020-02-25|Masimo Corporation|Soft boot pulse oximetry sensor| JP6808631B2|2015-02-06|2021-01-06|マシモ・コーポレイション|Combination of connector and sensor assembly| MX2017010046A|2015-02-06|2018-04-10|Masimo Corp|Fold flex circuit for optical probes.| US10342467B2|2015-03-11|2019-07-09|Nonin Medical, Inc.|Segmented sensor| US10524738B2|2015-05-04|2020-01-07|Cercacor Laboratories, Inc.|Noninvasive sensor system with visual infographic display| US10448871B2|2015-07-02|2019-10-22|Masimo Corporation|Advanced pulse oximetry sensor| CN108135503A|2015-08-11|2018-06-08|迈心诺公司|The medical monitoring analysis and playback of label including the light in response to being decayed by bodily tissue| KR20180044942A|2015-08-31|2018-05-03|마시모 코오퍼레이션|Wireless patient monitoring systems and methods| US10980423B2|2015-12-22|2021-04-20|University Of Washington|Devices and methods for predicting hemoglobin levels using electronic devices such as mobile phones| US10993662B2|2016-03-04|2021-05-04|Masimo Corporation|Nose sensor| US10537285B2|2016-03-04|2020-01-21|Masimo Corporation|Nose sensor| WO2017178889A1|2016-04-13|2017-10-19|Inspektor Research Systems B.V.|Bi-frequency dental examination| US11191484B2|2016-04-29|2021-12-07|Masimo Corporation|Optical sensor tape| WO2018009612A1|2016-07-06|2018-01-11|Patient Doctor Technologies, Inc.|Secure and zero knowledge data sharing for cloud applications| US10617302B2|2016-07-07|2020-04-14|Masimo Corporation|Wearable pulse oximeter and respiration monitor| US11076777B2|2016-10-13|2021-08-03|Masimo Corporation|Systems and methods for monitoring orientation to reduce pressure ulcer formation| WO2018119239A1|2016-12-22|2018-06-28|Cercacor Laboratories, Inc|Methods and devices for detecting intensity of light with translucent detector| US10721785B2|2017-01-18|2020-07-21|Masimo Corporation|Patient-worn wireless physiological sensor with pairing functionality| US11086609B2|2017-02-24|2021-08-10|Masimo Corporation|Medical monitoring hub| US10327713B2|2017-02-24|2019-06-25|Masimo Corporation|Modular multi-parameter patient monitoring device| WO2018156648A1|2017-02-24|2018-08-30|Masimo Corporation|Managing dynamic licenses for physiological parameters in a patient monitoring environment| US10388120B2|2017-02-24|2019-08-20|Masimo Corporation|Localized projection of audible noises in medical settings| US11024064B2|2017-02-24|2021-06-01|Masimo Corporation|Augmented reality system for displaying patient data| WO2018165618A1|2017-03-10|2018-09-13|Masimo Corporation|Pneumonia screener| WO2018194992A1|2017-04-18|2018-10-25|Masimo Corporation|Nose sensor| US10918281B2|2017-04-26|2021-02-16|Masimo Corporation|Medical monitoring device having multiple configurations| USD835282S1|2017-04-28|2018-12-04|Masimo Corporation|Medical monitoring device| WO2018201078A1|2017-04-28|2018-11-01|Masimo Corporation|Spot check measurement system| USD835284S1|2017-04-28|2018-12-04|Masimo Corporation|Medical monitoring device| USD835285S1|2017-04-28|2018-12-04|Masimo Corporation|Medical monitoring device| USD835283S1|2017-04-28|2018-12-04|Masimo Corporation|Medical monitoring device| WO2018208616A1|2017-05-08|2018-11-15|Masimo Corporation|System for pairing a medical system to a network controller by use of a dongle| US11026604B2|2017-07-13|2021-06-08|Cercacor Laboratories, Inc.|Medical monitoring device for harmonizing physiological measurements| USD906970S1|2017-08-15|2021-01-05|Masimo Corporation|Connector| KR20200042911A|2017-08-15|2020-04-24|마시모 코오퍼레이션|Waterproof connector for non-invasive patient monitors| USD890708S1|2017-08-15|2020-07-21|Masimo 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法律状态:
2002-04-17| AS| Assignment|Owner name: COMERICA BANK-CALIFORNIA, CALIFORNIA Free format text: SECURITY INTEREST;ASSIGNOR:MASIMO CORPORATION;REEL/FRAME:012822/0200 Effective date: 20010629 | 2002-04-26| STCF| Information on status: patent grant|Free format text: PATENTED CASE | 2005-11-10| FPAY| Fee payment|Year of fee payment: 4 | 2006-01-24| CC| Certificate of correction| 2006-08-08| AS| Assignment|Owner name: MASIMO CORPORATION, CALIFORNIA Free format text: RELEASE BY SECURED PARTY;ASSIGNOR:COMERICA BANK;REEL/FRAME:018061/0752 Effective date: 20060728 | 2009-11-10| FPAY| Fee payment|Year of fee payment: 8 | 2013-11-12| FPAY| Fee payment|Year of fee payment: 12 | 2014-04-29| AS| Assignment|Owner name: JPMORGAN CHASE BANK, NATIONAL ASSOCIATION, ILLINOI Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNORS:MASIMO CORPORATION;MASIMO AMERICAS, INC.;REEL/FRAME:032784/0864 Effective date: 20140423 Owner name: JPMORGAN CHASE BANK, NATIONAL ASSOCIATION, ILLINOIS Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNORS:MASIMO CORPORATION;MASIMO AMERICAS, INC.;REEL/FRAME:032784/0864 Effective date: 20140423 | 2014-05-27| AS| Assignment|Owner name: JPMORGAN CHASE BANK, NATIONAL ASSOCIATION, ILLINOIS Free format text: CORRECTIVE ASSIGNMENT TO CORRECT THE NATURE OF CONVEYANCE PREVIOUSLY RECORDED AT REEL: 032784 FRAME: 0864. ASSIGNOR(S) HEREBY CONFIRMS THE SECURITY AGREEMENT;ASSIGNORS:MASIMO AMERICAS, INC.;MASIMO CORPORATION;REEL/FRAME:033032/0426 Effective date: 20140423 Owner name: JPMORGAN CHASE BANK, NATIONAL ASSOCIATION, ILLINOI Free format text: CORRECTIVE ASSIGNMENT TO CORRECT THE NATURE OF CONVEYANCE PREVIOUSLY RECORDED AT REEL: 032784 FRAME: 0864. ASSIGNOR(S) HEREBY CONFIRMS THE SECURITY AGREEMENT;ASSIGNORS:MASIMO AMERICAS, INC.;MASIMO CORPORATION;REEL/FRAME:033032/0426 Effective date: 20140423 | 2018-11-07| AS| Assignment|Owner name: MASIMO CORPORATION, CALIFORNIA Free format text: RELEASE BY SECURED PARTY;ASSIGNOR:JPMORGAN CHASE BANK, NATIONAL ASSOCIATION;REEL/FRAME:047443/0109 Effective date: 20180405 Owner name: MASIMO AMERICAS, INC., CALIFORNIA Free format text: RELEASE BY SECURED PARTY;ASSIGNOR:JPMORGAN CHASE BANK, NATIONAL ASSOCIATION;REEL/FRAME:047443/0109 Effective date: 20180405 |
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申请号 | 申请日 | 专利标题 US15092299P| true| 1999-08-26|1999-08-26|| US09/420,544|US6580086B1|1999-08-26|1999-10-19|Shielded optical probe and method| US09/798,764|US6388240B2|1999-08-26|2001-03-02|Shielded optical probe and method having a longevity indication|US09/798,764| US6388240B2|1999-08-26|2001-03-02|Shielded optical probe and method having a longevity indication| 相关专利
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