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二酰基甘油的构象受限类似物。29. 细胞对二酰基甘油内酯化学邮政编码进行分类以产生多样且具选择性的生物活性。

Conformationally constrained analogues of diacylglycerol. 29. Cells sort diacylglycerol-lactone chemical zip codes to produce diverse and selective biological activities.

作者信息

Duan Dehui, Sigano Dina M, Kelley James A, Lai Christopher C, Lewin Nancy E, Kedei Noemi, Peach Megan L, Lee Jeewoo, Abeyweera Thushara P, Rotenberg Susan A, Kim Hee, Kim Young Ho, El Kazzouli Saïd, Chung Jae-Uk, Young Howard A, Young Matthew R, Baker Alyson, Colburn Nancy H, Haimovitz-Friedman Adriana, Truman Jean-Philip, Parrish Damon A, Deschamps Jeffrey R, Perry Nicholas A, Surawski Robert J, Blumberg Peter M, Marquez Victor E

机构信息

Laboratory of Medicinal Chemistry, National Cancer Institute at Frederick, National Institutes of Health, 376 Boyles Street, Frederick, Maryland 21702, USA.

出版信息

J Med Chem. 2008 Sep 11;51(17):5198-220. doi: 10.1021/jm8001907. Epub 2008 Aug 13.

Abstract

Diacylglycerol-lactone (DAG-lactone) libraries generated by a solid-phase approach using IRORI technology produced a variety of unique biological activities. Subtle differences in chemical diversity in two areas of the molecule, the combination of which generates what we have termed "chemical zip codes", are able to transform a relatively small chemical space into a larger universe of biological activities, as membrane-containing organelles within the cell appear to be able to decode these "chemical zip codes". It is postulated that after binding to protein kinase C (PKC) isozymes or other nonkinase target proteins that contain diacylglycerol responsive, membrane interacting domains (C1 domains), the resulting complexes are directed to diverse intracellular sites where different sets of substrates are accessed. Multiple cellular bioassays show that DAG-lactones, which bind in vitro to PKCalpha to varying degrees, expand their biological repertoire into a larger domain, eliciting distinct cellular responses.

摘要

通过使用IRORI技术的固相方法生成的二酰基甘油内酯(DAG-内酯)文库产生了多种独特的生物活性。分子两个区域化学多样性的细微差异,二者结合产生了我们所称的“化学邮政编码”,能够将相对较小的化学空间转化为更大的生物活性领域,因为细胞内含有膜的细胞器似乎能够解码这些“化学邮政编码”。据推测,在与蛋白激酶C(PKC)同工酶或其他含有二酰基甘油反应性膜相互作用结构域(C1结构域)的非激酶靶蛋白结合后,形成的复合物会被导向不同的细胞内位点,在那里可以接触到不同的底物组。多种细胞生物测定表明,在体外与PKCα不同程度结合的DAG-内酯将其生物功能扩展到更大的领域,引发不同的细胞反应。

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