Method of producing pyrrolidine derivatives
专利摘要:
Pyrrolidine derivatives of the formula <IMAGE> (I) are prepared from gamma -amino- beta -hydroxybutyric acid which, after reaction with a silylating agent, is reacted, in the presence of an acid acceptor, with a halogen derivative of an ester of an aliphatic acid and then cyclized to give the corresponding N-alkoxy-carbonylalkyl derivative which is converted into the corresponding amide by treatment with ammonia or with a mono- or di-substituted amine. The compounds produced by the present invention improve learning memory and display a protecting effect against the E.E.G. consequence of an overdose of barbituates and against the reduced performance following brain damage (e.g. cerebral edema). 公开号:SU984407A3 申请号:SU782579300 申请日:1978-02-10 公开日:1982-12-23 发明作者:Монгуцци Риккардо;Пиффери Джорджо 申请人:И.С.Ф. С.П.А. (Фирма); IPC主号:
专利说明:
. (54) METHOD FOR OBTAINING PYRROLIDINE DERIVATIVES This invention relates to a process for the preparation of pyrrolidine derivatives, which are used as physiologically active substances in medicine. A known method for producing pyrrolidine derivatives of the general formula RO-p-J .xRi iCHaV ow; R, R is hydrogen, acyl, alkyl; where Ng and R are the same or different c are hydrogen, alkyl p is an integer from O to 2, meaning that a compound of the general formula -COOR HOV (CH2) jiCOOR where R is alkyl With -Co ,; p - has the specified value, subjected to heating in the aprotic an organic solvent in the presence of water, the resulting 2,4-diketone derivative of the formula (Syag) 1-СООн,, where R and p have the indicated meanings, hydrogenate the complex hydride with ) 0 to form the corresponding 4-hydroxy derivative, which is then treated with an aqueous solution of aimiac or a mono- or disubstituted amine. The yield of the target product 13,315 26.6% 1. The disadvantage of this method is the relatively low yield of the target product. The goal of the invention is to increase the yield of the target product. The goal is achieved by the method of obtaining pyrrolidine derivatives of the general formula 25 but-p-i. where n is 1 or 2; and R may be the same or different and represent a hydrogen atom, alkyl; denotes the center of asymmetry of the molecule, using a 4-hydroxy derivative of the general formula HO-R-, „-СООВз where n is 1 or 2; alkyl, trichlorophenyl, monoyl. disubstituted amine of the formula .j where R and R may be the same or different and represent a water atom of the genus, alkyl with the proviso that the ab cannot simultaneously be hydrogen, as enantiomers or mixtures thereof, or an aqueous solution of ammonia, according to which α-amino-oxybutyric acid, taken as an individual enantiomer or mixture of enantiomers, is reacted with hexamethylenedisilazane at boiling point in anhydrous acetonitrile, the product thus obtained is treated with halo ester and the general formula Hae (CHii) nCOOR7,, Cvii) where NaB is bromine, chlorine, iodine; p and Rt, have the indicated values, at 30-80s in the presence of pr-propylene oxide, the resulting silyl derivative of the general formula CH5-SiO-p1 CH / N (CH2) „COOS3 where n, R3 and 1 has the indicated value is subjected to hydrolysis to obtain of the corresponding 4-hydroxy derivative which is reacted with a mono- or disubstituted amine of the general formula K, NHR / where R and R have the indicated meanings or aqueous ammonia, Example 1. 2- (4-hydroxypyrrole DIN-2-OH-1-IL) - ethyl acetate, 28 ml of hexamethyldisilylazan and 3 drops of trimethylchlorosilane were added to 10 g of T-amino-3-hydroxybutyloyl cells in 100 ml ezvodnogo la acetone. The reaction mixture is heated under reflux in a stream of nitrogen until a clear solution is obtained. The mixture was cooled to ambient temperature and 50 ml of propylene oxide was added thereto, followed by the addition of 9.4 ml of ethyl bromoacetate. The reaction mixture is heated under reflux for 15 hours, cooled to room temperature, and then evaporated in vacuo to a dry residue. The resulting residue contains crude 2- (4-trimethylsilyloxypyrrolidin-2-OH-1-IL) -ethyl acetate, which is purified by chromatography on a silica gel column by elution using ethyl acetate as an eluent. 8 g of 2- (4-oxyprolidin-2-on-1-yl) ethyl acetate are obtained in the form of a colorless oil, b.p. 180c at a pressure of 0.8 mm Hg. st, Example 2, 2- (4-hydroxypyrrolidine-2-OH-1-IL) -acetamide. A solution of 7.1 g of 2- (4-hydroxypyrrolidin-2-OH-4-IL) -ethyl acetate obtained in Example 1 in 7.1 ml of a solution of ammonium hydroxide (90) is stirred at room temperature for 15 hours. The reaction mixture is then diluted with 40 ml of acetone and continued stirring at room temperature until the solid precipitates out as white crystals. Hardening and drying are obtained by filtration by suction and drying 5.1 g (43%) 2- {4-hydroxypyrrolidin-2-one-1-yl) -acetamide, m.p. 160-162C; R 0.32 on silica gel (eluent acetonitrile - water in a ratio of 4: 1 by volume). Example 3, R (+) - 2- (4-hydroxypyrrolidin-2-one-1-yl) -acetamide, the process is carried out similarly to example 2, and as starting materials use H (-) - d-amino- | 5- hydroxybutyric acid and, respectively, R (+) - 2- (4-oxyprolipin-2-one-1-yl) - ethyl acetate (t, boiling pressure 0.8 mm Hg, cent.) and then R (+) - 2- (4-hydroxypyrrolidin-2-one-1-yl) -acetamide (so kip. 135136cjl i3 - (+} 36, (iodine, s, Example 4. 3- (4-Hydroxypyrolidine-2-OH -1-IL) -propionamide. The process is carried out analogously to example 2, but using ethyl-3-bromopropionate instead of ethyl bromoacetate, in this case, firstly 3- (4-oxyg pyrrolidin-2-one-1-yl) -e is obtained tilpropionat (t.kip, with decomposition 190s at a pressure (T, 8 mm Hg), and then 3- (4-OXYPYRROLIDIN-2-OH-1-IL) -propionamide (t.p. 99-100s) Yield of product 40%. Example 5. K-ethyl-2- (4-hydroxypyrrolidin-2-he-1-yl) -acetamide. / The process is carried out analogously to example 1, but using trichlbrphenyl bromoacetate instead of ethyl bromoacetate. 2- (4-hydroxypyrrolidin-2-one-1-yl) -trichlorophenylacetate is obtained. 5 g of 2- (4-oxypiperidine-2-one-1-yl) -trichlorphenylacetate is dissolved in 100 ml of methanol, the solution is cooled down and 10 ml of ethylamine is added to it. The reaction mixture is kept at room temperature for 48 hours, evaporated to dryness, and chromatographed to obtain 0.4 g of H-ethyl-2- (4-hydroxypropolidin-2-on-1-yl) acetamide; m.p. Rr 0.23 (solution for elution with ethyl acetate).
权利要求:
Claims (1) [1] Invention Formula about The method of obtaining pyrrolidine derivatives of the general formula BUT -"one (sa-som; Vg where n is 1 or 2; RY and Ri may be the same or different and represent 1 hydrogen atom, alkyl g; denotes the center of asymmetry of the molecule, using a 4-hydroxy derivative of the general formula BUT -t: I, --BI . (CRaU-CON where n is 1 or 2; Rj alkyl, trichlorophenyl, mono- or disubstituted amine of formula R NHR 2., where R and R 2. may be the same or different and represent a hydrogen atom, an alkyl, provided that both cannot be hydrogen at the same time, in the form of enantiomers or their mixture, or an aqueous solution of ammonia, which is characterized by the fact that, in order to increase the yield, an aL-amino-p-hydroxy-oil dislot taken in 0 as an individual enantiomer or as a mixture of enantiomers, is reacted with s-hexamethylene disilazane at the boiling point in anhydrous acetonitrile in the presence of trimethylchlorosilane, the product thus obtained is treated with the ester halo esters of the general formula e (SNG) ISOOYag, 0 where Hat is bromine, chlorine, iodine; p and R have the indicated values, at 30-80 seconds in the presence of propylene oxide, the resulting silyl derivatives of the general formula SNZ CH5-810 iCHs (СН2) „- СООК5 R and. where n, have the indicated meanings five hydrolyzed to form the corresponding 4-hydroxy derivative, which is reacted with a mono- or disubstituted amine of the general formula. 0 .2 where R and R2 have the indicated values or aqueous ammonia. Information sources, 5 taken into account in the examination 1, Patent of the USSR in application number 2388323 / 23-04, cl. C 07 D 207/12, 13,08,75 (prototype).
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同族专利:
公开号 | 公开日 NO147751B|1983-02-28| GB1588074A|1981-04-15| YU30378A|1982-10-31| FI66847C|1984-12-10| DK155279C|1989-07-24| YU40322B|1985-12-31| NL187207C|1991-07-01| PL108024B1|1980-03-31| HU178588B|1982-05-28| FI780406A|1978-08-12| JPS53101368A|1978-09-04| NO780463L|1978-08-14| CH631703A5|1982-08-31| SE428208B|1983-06-13| DE2759033C2|1984-04-19| PT67641B|1980-03-03| NL187207B|1991-02-01| PL204550A1|1978-12-04| DK155279B|1989-03-20| PT67641A|1978-03-01| DE2759033A1|1978-08-17| IN147764B|1980-06-21| US4124594A|1978-11-07| NL7801501A|1978-08-15| ATA88778A|1980-11-15| CA1083585A|1980-08-12| AR219734A1|1980-09-15| DK63078A|1978-08-12| ES466857A1|1978-10-01| SE7801537L|1978-08-12| NO147751C|1983-06-08| CS214767B2|1982-05-28| FI66847B|1984-08-31| IT1075564B|1985-04-22| JPS6338349B2|1988-07-29| AT362781B|1981-06-10| MX4988E|1983-01-31|
引用文献:
公开号 | 申请日 | 公开日 | 申请人 | 专利标题 AR211398Q|1975-08-13|1977-12-15|Isf Spa|A PROCEDURE FOR PREPARING -ACILAMIDE DERIVATIVES| IT1045043B|1975-08-13|1980-04-21|Isf Spa|PYROLIDINE DERIVATIVES|US2858573A|1958-11-04|Fibers | IT1141287B|1979-06-13|1986-10-01|Nattermann A & Cie|PYROLIDIN ACIDS AMIDS--ON--ILALKYL-CARBOXYLS, PROCEDURE FOR THEIR PREPARATION AND MEDICINAL PRODUCTS CONTAINING THEM| FR2515179B1|1981-07-24|1985-01-18|Hoffmann La Roche| IT1206699B|1984-02-27|1989-04-27|Isf Spa|PROCEDURE FOR PREPARING PYROLIDONE DERIVATIVES.| IT1173768B|1984-04-02|1987-06-24|Isf Spa|PREPARATION PROCEDURE FOR 1-CARBAMOYLMETHYL DERIVATIVES OF 4-HYDROXY-2-BONE-PYROLIDINE AS WELL AS INTERMEDIATES TO OBTAIN SUCH COMPOUNDS| CH666483A5|1985-01-16|1988-07-29|Lonza Ag|METHOD FOR PRODUCING Thiotetronic acid.| IT1190378B|1985-06-21|1988-02-16|Isf Spa|PYROLIDONIC DERIVATIVES| US4686296A|1985-07-26|1987-08-11|Denki Kagaku Kogyo Kabushiki Kaisha|Process for producing oxiracetam| IL80071D0|1985-09-24|1986-12-31|Lonza Ag|Pyrrolidine acetamide derivatives| HU195773B|1985-09-24|1988-07-28|Lonza Ag|Process for preparing alkyl esters of 4-alkoxy-3-pyrrolin-2-on-1-yl-acetic acid| CH668423A5|1986-06-19|1988-12-30|Lonza Ag|METHOD FOR PRODUCING 4-ALKOXY-3-pyrroline-2-ONES.| CH668422A5|1986-06-26|1988-12-30|Lonza Ag|4-BENZYLOXY-3-PYRROLIN-2-ON, THE PRODUCTION AND USE THEREOF FOR THE SYNTHESIS OF TETRAMIC ACID.| CH668424A5|1986-06-26|1988-12-30|Lonza Ag|4-BENZYLOXY-3-PYRROLIN-2-ON-L-YL-ACETAMIDE, THE PRODUCTION AND USE THEREOF.| CH667655A5|1986-09-24|1988-10-31|Lonza Ag|METHOD FOR PRODUCING 4-ALKOXY-2THIOPHENONES.| CH670644A5|1986-12-18|1989-06-30|Lonza Ag| EP0358128B1|1988-09-06|1995-06-28|Lonza Ag|Process for the preparation of 5-alkyltetramic acids| FI95034C|1989-03-15|1995-12-11|Lonza Ag|Process for the preparation of 1,3-substituted tetrahydro-1H-thieno [3,4-d] imidazol-2-one-4-ylidenepentanoic acid ester| CH680293A5|1990-06-26|1992-07-31|Lonza Ag| CN101704778B|2009-09-30|2012-10-17|厦门市华兴化工有限公司|Method for preparing 4-hydroxyl yrrolidone-2-acetamide| WO2011143872A1|2010-05-21|2011-11-24|重庆润泽医疗器械有限公司|Crystal form of -4-hydroxy-2-oxo-1-pyrrolidine acetamide, preparation method and use thereof| CN107973739B|2016-10-24|2020-03-20|重庆润泽医药有限公司|Dextro-oxiracetam crystal form II and preparation method and application thereof| EP3530650A4|2016-10-24|2020-03-25|Chongqing Runze Pharmaceutical Company Limited|Crystalline form of -4-hydroxy-2-oxo-1-pyrrolidineacetamide, preparation method therefor and use thereof| US10696629B2|2016-10-24|2020-06-30|Chongqing Runze Pharmaceutical Company Limited|Crystalline form of dextral oxiracetam, preparation method therefor and use thereof| CN108299267A|2017-01-12|2018-07-20|重庆润泽医药有限公司| crystal form and its preparation method and application of -4- hydroxyls -2- oxygen -1- pyrrolidine acetamides| CN108299268A|2017-01-12|2018-07-20|重庆润泽医药有限公司|The preparation method of one kind-4- hydroxyl -2- oxygen -1- pyrrolidine acetamide crystal forms|
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申请号 | 申请日 | 专利标题 IT20226/77A|IT1075564B|1977-02-11|1977-02-11|PROCEDURE FOR THE PREPARATION OF PYROLIDINE DERIVATIVES| 相关专利
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