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14 条记录 (耗时 0.021 秒)

    Production method of epoxide crystal
    1.
    发明授权
    Production method of epoxide crystal 失效
    环氧化物晶体的制备方法

    公开(公告)号:US06764545B2

    公开(公告)日:2004-07-20

    申请号:US10011304

    申请日:2001-12-11

    申请人: Yuichi Suzuki Naoko Hirose Tomoyuki Onishi Kunisuke Izawa

    发明人: Yuichi Suzuki Naoko Hirose Tomoyuki Onishi Kunisuke Izawa

    IPC分类号: C30B708

    CPC分类号: C07D301/36

    摘要: The present invention provides a production method including adding water to a solution of (2R,3S)-3-tert-butoxycarbonylamino-1,2-epoxy-4-phenylbutane ((2R,3S)-epoxide compound) or (2S,3R)-3-tert-butoxycarbonylamino-1,2-epoxy-4-phenylbutane ((2S,3R)-epoxide compound) in a polar solvent to allow crystallization, whereby to produce crystals of the (2R,3S)-epoxide compound or the (2S,3R)-epoxide compound conveniently in a high yield by an industrial production method without requiring an extremely low temperature.

    摘要翻译: 本发明提供一种制备方法,其包括向(2R,3S)-3-叔丁氧基羰基氨基-1,2-环氧-4-苯基丁烷((2R,3S) - 环氧化合物)或(2S,3R )-3-叔丁氧基羰基氨基-1,2-环氧-4-苯基丁烷((2S,3R) - 环氧化合物)在极性溶剂中进行结晶,从而得到(2R,3S) - 环氧化合物的晶体或 (2S,3R) - 环氧化合物通过工业生产方法方便地高收率,而不需要极低的温度。

    Processes for preparation of N-protected-β-amino alcohols and N-protected-β-amino epoxides
    2.
    发明授权
    Processes for preparation of N-protected-β-amino alcohols and N-protected-β-amino epoxides 失效
    制备N-保护的β-氨基醇和N-保护的β-氨基环氧化物的方法

    公开(公告)号:US07122696B2

    公开(公告)日:2006-10-17

    申请号:US10432353

    申请日:2001-11-30

    申请人: Naoko Hirose Tomoyuki Onishi Daigaku Hideura Yasuyuki Otake Kunisuke Izawa

    发明人: Naoko Hirose Tomoyuki Onishi Daigaku Hideura Yasuyuki Otake Kunisuke Izawa

    IPC分类号: C07C261/00

    CPC分类号: C07D303/36 C07B2200/07 C07C269/08 C07C271/16

    摘要: Herein are disclosed a process for increasing in purity, or purifying, an N-protected-β-aminoalcohol which process comprises (i) adding water to a polar organic solvent in which an N-protected-β-aminoalcohol such as a (2R,3S)- or (2S,3R)-3-tert-butoxycarbonylamino-1-halo-2-hydroxy-4-phenylbutane or the like, or (ii) crystallizing such an N-protected-β-aminoalcohol from a diol or a diol-based mixed solvent, and a process for producing the corresponding N-protected-β-aminoepoxide which process comprises treating, with a base, the thus purity-enhanced N-protected-β-aminoalcohol. Such N-protected-β-aminoalcohols and N-protected-β-aminoepoxides are both useful as synthetic intermediates for medicine compounds, such as, e.g., HIV protease inhibitor and the like.

    摘要翻译: 本文公开了提高纯度或纯化N-保护的β-氨基醇的方法,该方法包括(i)向极性有机溶剂中加入水,其中N-保护的β-氨基醇如(2R, 3S) - 或(2S,3R)-3-叔丁氧基羰基氨基-1-卤代-2-羟基-4-苯基丁烷等,或(ii)将这种N-保护的β-氨基醇从二醇或 二醇基混合溶剂,以及生产相应的N-保护的β-氨基环氧化物的方法,该方法包括用碱处理如此纯度增强的N-保护的β-氨基醇。 这种N-保护的β-氨基醇和N-保护的β-氨基环氧化物都可用作药物化合物的合成中间体,例如HIV蛋白酶抑制剂等。

    Method for producing epoxide crystal
    9.
    发明授权
    Method for producing epoxide crystal 失效
    环氧化物晶体的制备方法

    公开(公告)号:US06765100B2

    公开(公告)日:2004-07-20

    申请号:US09973191

    申请日:2001-10-10

    申请人: Tomoyuki Onishi Naoko Hirose Yasuyuki Otake Takashi Nakano Yutaka Honda Masakazu Nakazawa Kunisuke Izawa

    发明人: Tomoyuki Onishi Naoko Hirose Yasuyuki Otake Takashi Nakano Yutaka Honda Masakazu Nakazawa Kunisuke Izawa

    IPC分类号: C07D30124

    CPC分类号: C07C269/06 C07B2200/07 C07C269/08 C07D263/24 C07D303/36 C07C271/16

    摘要: The invention relates to a method for industrially producing highly pure (2R, 3S)- or (2S, 3R)-N-carbamate-protected &bgr;-aminoepoxide (crystal) or (2R, 3S)- or (2S, 3R)-N-carbamate-protected &bgr;-aminoalcohol. The method for producing N-carbamate-protected &bgr;-aminoepoxide crystal, includes one or more of the following steps (a) to (d): (a) dissolving (2R, 3S)- or (2S, 3R)-N-carbamate-protected &bgr;-aminoalcohol containing at least the diastereomer as an impurity in a solvent including at least one or more selected from aromatic hydrocarbon solvent, saturated hydrocarbon solvent, aqueous mixture solvent, acetone and 2-propanol, to remove insoluble matters; (b) treating the (2R, 3S)- or (2S, 3R)-N-carbamate-protected &bgr;-aminoalcohol with a base, thereby converting the N-carbamate-protected &bgr;-aminoalcohol to (2R, 3S)- or (2S, 3R)-N-carbamate-protected &bgr;-aminoepoxide; (c) treating the (2R, 3S)- or (2S, 3R)-N-carbamate-protected &bgr;-aminoepoxide containing at least the diastereomer as an impurity with an acid, thereby converting the diastereomer as an impurity to (4S, 5R) or (4R, 5S) oxazolidin-2-one derivative, and optionally separating and removing the resulting oxazolidin-2-one derivative in water or an aqueous mixture solvent; and (d) crystallizing the (2R, 3S)- or (2S, 3R)-N-carbamate-protected &bgr;-aminoepoxide in a mixture solvent of water and water-miscible organic solvent. By the methods of the present invention, highly pure (2R, 3S)- or (2S, 3R)-N-carbamate-protected &bgr;-aminoepoxide or (2R, 3S) or (2S, 3R)-N-carbamate-protected &bgr;-aminoalcohol can be efficiently produced.

    摘要翻译: 本发明涉及工业生产高纯度(2R,3S) - 或(2S,3R)-N-氨基甲酸酯保护的β-氨基环氧化物(晶体)或(2R,3S) - 或(2S,3R)-N 氨基甲酸酯保护的β-氨基醇。 制备N-氨基甲酸酯保护的β-氨基环氧化物晶体的方法包括一个或多个以下步骤(a)至(d):( a)将(2R,3S) - 或(2S,3R)-N-氨基甲酸酯 在包含至少一种或多种选自芳族烃溶剂,饱和烃溶剂,含水混合物溶剂,丙酮和2-丙醇的溶剂的溶剂中至少含有作为杂质的非对映体的β-保护的β-氨基醇,以除去不溶物;(b) 用碱处理(2R,3S) - 或(2S,3R)-N-氨基甲酸酯保护的β-氨基醇,从而将N-氨基甲酸酯保护的β-氨基醇转化为(2R,3S) - 或(2S,3R )-N-氨基甲酸酯保护的β-氨基环氧化物;(c)用酸处理至少含有非对映体作为杂质的(2R,3S) - 或(2S,3R)-N-氨基甲酸酯保护的β-氨基环氧化物,由此 将非对映异构体作为杂质转化为(4S,5R)或(4R,5S)恶唑烷-2-酮衍生物,任选分离和除去得到的恶唑烷-2-酮衍生物 在水或含水混合溶剂中; 和(d)在水和水混溶性有机溶剂的混合溶剂中结晶(2R,3S) - 或(2S,3R)-N-氨基甲酸酯保护的β-氨基环氧化物。 通过本发明的方法,高纯度(2R,3S) - 或(2S,3R)-N-氨基甲酸酯保护的β-氨基环氧化物或(2R,3S)或(2S,3R)-N-氨基甲酸酯保护的β - 氨基醇可以有效地生产。

    Methods for producing nucleoside derivatives and intermediates therefor
    10.
    发明授权
    Methods for producing nucleoside derivatives and intermediates therefor 失效
    制备核苷衍生物的方法及其中间体

    公开(公告)号:US6090937A

    公开(公告)日:2000-07-18

    申请号:US267789

    申请日:1999-03-15

    申请人: Satoshi Takamatsu Satoshi Katayama Naoko Hirose Kunisuke Izawa Tokumi Maruyama

    发明人: Satoshi Takamatsu Satoshi Katayama Naoko Hirose Kunisuke Izawa Tokumi Maruyama

    IPC分类号: C07D473/00 C07H19/16 C07H19/167 C07H19/19

    CPC分类号: C07D473/00 C07H19/16

    摘要: Novel intermediates of nucleoside derivatives, of which the 6-position of the nucleic acid base moiety is substituted with a halogen atom, are produced. Using those novel intermediates, even substrates, of which the 3'-position of the saccharide moiety is deoxylated, can be substituted at the 2'-position at an extremely high yield. Specifically, by subjecting a 3'-deoxy derivative of inosine to 6-halogenation to give a 6-halide of the derivative, and then subjecting it to 2'-deoxylation/substitution with a fluorine atom or the like, followed by further subjecting it to substitution with an amino group, a hydroxyl group or any other intended substituent at the 6-positioned halogen atom, nucleoside derivatives are produced at a high yield.Methods for producing nucleoside derivatives including 9-(2,3-dideoxy-2-fluoro-.beta.-D-threo-pentofuranosyl)adenine (FddA) and their related compounds, in a simplified manner, at a high yield and at low costs, and especially Economical methods for substituting substrates, of which the 3'-position of the saccharide moiety is deoxylated, at the 2'-position to produce those nucleoside derivatives on an industrial scale are also provided.

    摘要翻译: 产生其核酸碱基部分的6位被卤素原子取代的核苷衍生物的新型中间体。 使用这些新型中间体,其中糖基部分的3'-位脱氧的偶联底物可以在2'-位以非常高的收率被取代。 具体来说,通过使肌苷的3'-脱氧衍生物进行6-卤化,得到该衍生物的6-卤化物,然后用氟原子等进行2'-脱氧/取代,然后进一步对其进行 以6-取代的卤素原子被氨基,羟基或任何其它目的取代基取代,以高产率生产核苷衍生物。 以简单的方式以高产率和低成本生产包括9-(2,3-二脱氧-2-氟-β-D-苏氨酸 - 呋喃鸟糖基)腺嘌呤(FddA)及其相关化合物的核苷衍生物的方法, 并且还提供了用于将2'-位上的糖部分的3'-位脱氧的底物替代为工业规模生产这些核苷衍生物的经济方法。