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公开(公告)号:US5707837A
公开(公告)日:1998-01-13
申请号:US696805
申请日:1996-08-09
IPC分类号: C12P13/06 , C07C229/08 , C12P41/00 , C12P13/04
CPC分类号: C12P41/009
摘要: A method is disclosed by which N-carbamoyl-(R)-tert.-leucine is obtained from tert-butyl hydantoin by means of an (R)-specific hydantoinase, in which N-carbamoyl-(R)-tert.-leucine is converted by reaction with nitrite or an (R)-carbamoylase to (R)-tert-leucine.
摘要翻译: 公开了通过(R) - 特异性乙内酰脲酶从N-叔丁基乙内酰脲得到N-氨基甲酰基 - (R) - 亮氨酸的方法,其中N-氨基甲酰基 - (R) - 亮氨酸 通过与亚硝酸盐或(R) - 氨基甲酰基酶与(R) - 亮氨酸反应转化。
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2.发明授权Method of preparing amionoakylhydantoins and aminoalkyl-alpha-amino acids 失效制备酰氨基乙酰乙内酰脲和氨基烷基-α-氨基酸的方法
公开(公告)号:US5608076A
公开(公告)日:1997-03-04
申请号:US416855
申请日:1995-05-23
IPC分类号: C07C227/24 , C07C227/30 , C07C229/26 , C07D233/72 , C07D233/76 , A61K31/415
CPC分类号: C07C227/24 , C07D233/76 , Y02P20/55
摘要: The invention relates to a method of preparing 5-(aminoalkyl)-hydantoins with basic side chain in which the protection of the amino function in the side chain is necessary during the formation of the hydantoin requires minimal expense.
摘要翻译: PCT No.PCT / EP93 / 02753 Sec。 371日期:1995年5月23日 102(e)日期1995年5月23日PCT提交1993年10月8日PCT公布。 出版物WO94 / 08974 日本1994年4月28日本发明涉及一种制备具有碱性侧链的5-(氨基烷基) - 乙内酰脲的方法,其中在形成乙内酰脲期间保护侧链中的氨基功能是必需的,需要最少的费用。
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公开(公告)号:US06251625B1
公开(公告)日:2001-06-26
申请号:US09011859
申请日:1998-04-03
IPC分类号: C12P2106
摘要: The invention concerns a process for the enzymatic preparation of protected di- and oligopeptides and the separation of the protective groups used. The process according to the invention enables peptides to be synthesized simply and economically and the protective group to be separated carefully. The process comprises three reaction steps: 1. Preparation of N-carbamoyl amino acid or N-carbamoyl amino acid derivatives; 2. Formation of the peptide bond between the carbamoyl-protected electrophile and nucelophile; and 3. Separation of the carbamoyl-protective group.
摘要翻译: 本发明涉及用于酶制备受保护的二肽和寡肽以及所用保护基的分离的方法。 根据本发明的方法使得肽可以简单和经济地合成,并且保护基被仔细分离。 该方法包括三个反应步骤:1.制备N-氨基甲酰基氨基酸或N-氨基甲酰基氨基酸衍生物; 氨基甲酰基保护的亲电子和生物素之间的肽键的形成; 和3.氨基甲酰基保护基的分离。
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公开(公告)号:US5994555A
公开(公告)日:1999-11-30
申请号:US138340
申请日:1998-08-21
IPC分类号: C07B53/00 , C07C269/04 , C07C271/22 , C07D217/26 , C07D263/06 , C07D263/20 , C07D263/24 , C07D413/06
CPC分类号: C07D263/20 , C07C271/22 , C07D217/26 , C07D263/24 , C07D413/06
摘要: A process for producing 2-[3(S)-amino-2-(R)-hydroxyl-4-phenyl butyl]-N-tert,butyl decahydro-(4aS,8aS)-isoquinoline-e(S)-carboxamide of the formula (I) via 3(S)-[lower alkoxy carbonyl amino, phenoxy carbonyl amino or benzyl oxycarbonyl amino]-2-hydroxy-4-phenyl butyric acid and process for producing said acid.
摘要翻译: 制备2- [3(S) - 氨基-2-(R) - 羟基-4-苯基丁基] -N-叔丁基十氢 - (4aS,8aS) - 异喹啉e(S) - 甲酰胺的方法 式(I)通过3(S) - [低级烷氧基羰基氨基,苯氧基羰基氨基或苄基氧羰基氨基] -2-羟基-4-苯基丁酸,以及制备所述酸的方法。
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5.发明授权Method of isolating 1-�N.sup.2 -((S)-ethoxycarbonyl)-3-phenylpropyl)-N.sup.6 -trifluoroacetyl!-L-lysyl-L-proline (lisinopril (TFA) ethyl ester, LPE) 失效分离1- [N 2 - ((S) - 乙氧羰基)-3-苯基丙基)-N6-三氟乙酰基] -L-赖氨酰-L-脯氨酸(赖诺普利(TFA)乙酯,LPE)
公开(公告)号:US5907044A
公开(公告)日:1999-05-25
申请号:US951579
申请日:1997-10-16
IPC分类号: C07K1/30 , A61K38/00 , C07K5/02 , C07K5/068 , C07D207/20 , C07D207/12
CPC分类号: C07K5/0222 , A61K38/00
摘要: A method of isolating 1-�N.sup.2 -((S)-ethoxycarbonyl)-3-phenylpropyl)-N.sup.6 -trifluoroacetyl!-L-lysyl-L-proline (lisinopril (TFA) ethyl ester, LPE). The solvent or solvent mixture used for the extraction is also a main constituent of the solvent or solvent mixture from which the crystallization takes place. High yield as well as good purity of the end product are obtained, without distillation. 1-�N.sup.2 -((S)-ethoxycarbonyl)-3-phenylpropyl)-N.sup.6 -trifluoroacetyl!-L-lysyl-L-proline (lisinopril (TFA) ethyl ester, LPE) is described as a precursor for producing an ACE inhibitor.
摘要翻译: 分离1- [N 2 - ((S) - 乙氧基羰基)-3-苯基丙基)-N6-三氟乙酰基] -L-赖氨酰-L-脯氨酸(赖诺普利(TFA)乙酯,LPE)的方法。 用于萃取的溶剂或溶剂混合物也是发生结晶的溶剂或溶剂混合物的主要成分。 无需蒸馏即可获得最终产物的高产率和良好的纯度。 1- [N 2 - ((S) - 乙氧基羰基)-3-苯基丙基)-N6-三氟乙酰基] -L-赖氨酰-L-脯氨酸(赖诺普利(TFA)乙酯,LPE)被描述为制备ACE抑制剂的前体 。
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公开(公告)号:US5631385A
公开(公告)日:1997-05-20
申请号:US671535
申请日:1996-06-27
IPC分类号: A61K31/40 , A61K31/401 , A61P9/12 , C07D207/24 , C07D495/10 , C07D207/46
CPC分类号: C07D207/24
摘要: Method for the preparation of N-protected 4-ketoproline derivatives of formula I ##STR1## by oxidation of the corresponding N-protected 4-hydroxyproline derivatives of ##STR2## using the system TEMPO (2,2,6,6-tetramethylpiperidinyl oxy free radical)/NaOCl.
摘要翻译: 通过使用系统TEMPO(2,2,6,6)氧化相应的N-保护的式III的4-羟基脯氨酸衍生物,制备式I的N-保护的4-酮咯啉衍生物的方法 - 四甲基哌啶基氧基自由基)/ NaOCl。
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7.发明授权Transesterification and other conversion reactions of acid derivatives, using an amidine base 失效酸衍生物的酯交换和其他转化反应,使用脒碱
公开(公告)号:US6090913A
公开(公告)日:2000-07-18
申请号:US826258
申请日:1997-03-27
IPC分类号: C07C67/03 , B01J27/24 , C07B41/12 , C07B43/06 , C07C69/614 , C07K1/00 , C07K1/02 , C07K1/04 , C07K1/113 , C07K1/12 , C07K5/06 , C07K5/08 , C07K5/10 , C07C67/02
摘要: A process employs amidine or amidine base and a metal compound in the presence of an alcohol or water to transesterify, or saponify esters or amides. Since the process employs relatively mild conditions, it is especially suitable for the production of optically active substances and biomolecules, e.g. peptides, amino acids and nucleic acids which are sensitive to elevated temperatures, extreme pH values and/or long reaction times since these compounds are easily racemised or denatured. The conditions additionally find use in solid phase systems. When amino acid or peptide esters are saponified, the splitting is brought about with lithium hydroxide alone under mild conditions. The use of an amidine base, more particularly DBU or DBN, in combination with the metal salt additionally accelerates the reaction so strongly that even sensitive acid derivatives can be reacted under mild conditions. The amidine based system lends itself to the manufacture of complex esters, gentle splitting of peptides from the carrier, gentle saponification of amides or esters.
摘要翻译: 一种方法是在醇或水的存在下使用脒或脒碱和金属化合物来酯化或酯化酯或酰胺。 由于该方法采用相对温和的条件,所以特别适用于生产光学活性物质和生物分子,例如, 对升高的温度,极端的pH值和/或较长的反应时间敏感的肽,氨基酸和核酸,因为这些化合物容易外消旋或变性。 条件另外可用于固相系统。 当氨基酸或肽酯被皂化时,在温和条件下单独用氢氧化锂进行裂解。 使用脒碱,更特别是DBU或DBN与金属盐组合,另外加速反应,使得即使敏感的酸衍生物也可在温和的条件下反应。 基于脒的系统适用于复杂酯的制造,肽从载体的温和分裂,温和皂化酰胺或酯。
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公开(公告)号:US5744611A
公开(公告)日:1998-04-28
申请号:US793702
申请日:1997-03-03
IPC分类号: C07D263/24 , C07C213/00 , C07C215/02 , C07C215/08 , C07C215/10 , C07C215/28 , C07D263/20
CPC分类号: C07D263/20 , C07C213/00 , C07C215/08 , C07C215/10 , C07C215/28
摘要: A process is disclosed for reducing amino acids and derivatives thereof Compounds of formula (I), in which n=0 or 1 and R.sup.1, R.sup.2, R.sup.3, R.sup.4, R.sup.5 and R.sup.6 have the meanings given in the description, are reduced to the corresponding amino alcohols of formula (II): the formula (I) compounds are converted in a first step, in at least one alcohol and with the addition of acid and heat to an ester, this process producing a reaction mixture containing the ester; the ester is converted in a second reaction step with alkali or alkaline earth borohydride to compounds of formula II. By specifying that the second step be carried out without isolating the ester from the reaction mixture and by using alkali or alkaline earth borohydrides which are not activated, the invention facilitates the production from amino acids and their derivatives of the correponding alcohols in a simple "single vessel" process, with high yields and in such a way as to preserve a given centre of chirality. Applications: synthesis components, preparation of optically active compounds splitting of racemic compounds. ##STR1##
摘要翻译: PCT No.PCT / EP95 / 03281 Sec。 371日期1997年3月3日 102(e)1997年3月3日PCT PCT 1996年8月17日PCT公布。 出版物WO96 / 07634 日本公开了1996年3月14日公开的用于还原氨基酸及其衍生物的方法式(I)化合物,其中n = 0或1,R1,R2,R3,R4,R5和R6具有说明书中给出的含义, 被还原成相应的式(II)的氨基醇:式(I)化合物在第一步中,在至少一种醇中转化,并加酸和加热至酯,该方法产生含有 酯; 该酯在与碱金属或碱土金属硼氢化物的第二反应步骤中转化为式II化合物。 通过规定第二步在不从反应混合物中分离出酯的情况下进行,并且通过使用未活化的碱金属或碱土金属硼氢化物,本发明便于以简单的“单一”形式从相应的醇的氨基酸及其衍生物生产 船只“过程,产量高,并且以保持给定的手性中心的方式。 应用:合成成分,外消旋化合物的旋光活性化合物的制备。 (I)
(II) -
9.发明授权Process for purifying 1-[N.sup.2 -((S)-ethoxycarbonyl)-3-phenylpropyl)-N.sup.6 -trifluoroacetyl]-l-lysyl-l-proline (lisinopril (TFA) ethyl ester 失效纯化1- [N 2 - ((S) - 乙氧基羰基)-3-苯基丙基)-N6-三氟乙酰基〕-1-赖酰基-1-脯氨酸(赖诺普利(TFA)乙酯)
公开(公告)号:US5616727A
公开(公告)日:1997-04-01
申请号:US616885
申请日:1996-03-18
CPC分类号: C07K5/0222 , A61K38/00
摘要: A process for purifying 1-[N.sup.2 -((S)-ethoxycarbonyl)-3-phenylpropyl)-N.sup.6 -trifluoroacetyl]-1-lysyl-1-proline by extraction and crystallization. The process includes a two step extraction in a two phase aqueous/organic solvent system and crystallization from organic solvent.
摘要翻译: 通过萃取和结晶纯化1- [N 2 - ((S) - 乙氧基羰基)-3-苯基丙基)-N6-三氟乙酰基] -1-赖氨酰-1-脯氨酸的方法。 该方法包括在两相水/有机溶剂系统中进行两步萃取并从有机溶剂中结晶。
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![1-[N2-((S)-ethoxycarbonyl)-3-phenylproply)-N6-trifluoroacetyl]-L-ysyl-L-proline (lisinopril (TFA) ethyl ester, LPE)](/abs-image/US/2002/09/24/US06455705B1/abs.jpg.150x150.jpg)
10.发明授权1-[N2-((S)-ethoxycarbonyl)-3-phenylproply)-N6-trifluoroacetyl]-L-ysyl-L-proline (lisinopril (TFA) ethyl ester, LPE) 失效-1- [N 2 - ((S) - 乙氧基羰基)-3-苯基丙基)-N6-三氟乙酰基] -L-甲酰基-L-脯氨酸(赖诺普利(TFA)乙酯,LPE)公开(公告)号:US06455705B1
公开(公告)日:2002-09-24
申请号:US09220693
申请日:1998-12-24
IPC分类号: C04D20722
CPC分类号: C07K5/0222 , A61K38/00
摘要: A method of isolating 1-[N2-((S)-ethoxycarbonyl)-3-phenylpropyl)-N6-trifluoroacetyl]-L-lysyl-L-proline (lisinopril (TFA) ethyl ester, LPE). The solvent or solvent mixture used for the extraction is also a main constituent of the solvent or solvent mixture from which the crystallization takes place. High yield as well as good purity of the end product are obtained, without distillation. 1-[N2-((S)-ethoxycarbonyl)-3-phenylpropyl)-N6-trifluoroacetyl]-L-lysyl-L-proline (lisinopril (TFA) ethyl ester, LPE) is described as a precursor for producing an ACE inhibitor.
摘要翻译: 分离1- [N 2 - ((S) - 乙氧基羰基)-3-苯基丙基)-N6-三氟乙酰基] -L-赖氨酰-L-脯氨酸(赖诺普利(TFA)乙酯,LPE)的方法。 用于萃取的溶剂或溶剂混合物也是发生结晶的溶剂或溶剂混合物的主要成分。 无需蒸馏即可获得最终产物的高产率和良好的纯度。 1- [N 2 - ((S) - 乙氧基羰基)-3-苯基丙基)-N6-三氟乙酰基] -L-赖氨酰-L-脯氨酸(赖诺普利(TFA)乙酯,LPE)被描述为制备ACE抑制剂的前体
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