Synthesis of cinnamic acids and related isosteres as potent and selective alphavbeta3 receptor antagonists.

Penning TD; Russell MA; Chen BB; Chen HY; Desai BN; Docter SH; Edwards DJ; Gesicki GJ; Liang CD; Malecha JW; Yu SS; Engleman VW; Freeman SK; Hanneke ML; Shannon KE; Westlin MM; Nickols GA

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Synthesis of cinnamic acids and related isosteres as potent and selective alphavbeta3 receptor antagonists.

机译：肉桂酸和相关的等位基因的合成，作为有效的和选择性的αvbeta3受体拮抗剂。

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We describe a series of conformationally-restricted cinnamic acid peptidomimetics as well as several cinnamic acid isosteres, including 3-phenylpropionic acids, 2-amino-3-phenylpropionic acids, phenoxyacetic acids and 2-phenylcyclopropylcarboxylic acids. Several analogues demonstrated low to sub-nanomolar potencies against alpha(v)beta(3) and greater than 200-fold selectivity against the other beta(3) integrin alpha(IIb)beta(3). In whole 293 cells, many of these analogues also showed modest selectivity against other alpha(v) integrins such as alpha(v)beta(1) and alpha(v)beta(5). These compounds were synthesized from readily available starting materials using either Heck or Mitsunobu coupling conditions.

机译：我们描述了一系列的构象受限的肉桂酸肽模拟物以及几种肉桂酸的异构体，包括3-苯基丙酸，2-氨基-3-苯基丙酸，苯氧基乙酸和2-苯基环丙基羧酸。几个类似物表现出对alpha（v）beta（3）的低至亚纳摩尔效价，对其他beta（3）整联蛋白alpha（IIb）beta（3）的选择性大于200倍。在整个293细胞中，许多类似物还表现出对其他alpha（v）整联蛋白如alpha（v）beta（1）和alpha（v）beta（5）的适度选择性。这些化合物是使用Heck或Mitsunobu偶联条件由易于获得的起始原料合成的。

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来源
《Bioorganic and Medicinal Chemistry Letters》 |2004年第6期|共6页
作者
Penning TD; Russell MA; Chen BB; Chen HY; Desai BN; Docter SH; Edwards DJ; Gesicki GJ; Liang CD; Malecha JW; Yu SS; Engleman VW; Freeman SK; Hanneke ML; Shannon KE; Westlin MM; Nickols GA;
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正文语种 eng
中图分类基础医学;
关键词
cinnamic acid; Synthesis; receptor;

机译：肉桂酸合成受体;

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1. Synthesis of cinnamic acids and related isosteres as potent and selective alphavbeta3 receptor antagonists. [J] . Penning TD, Russell MA, Chen BB, Bioorganic and Medicinal Chemistry Letters . 2004,第6期

机译：肉桂酸和相关的等位基因的合成，作为有效的和选择性的αvbeta3受体拮抗剂。
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Synthesis of cinnamic acids and related isosteres as potent and selective alphavbeta3 receptor antagonists.

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