Synthesis and Biological Investigation of Δ~(12)-Prostaglandin J_3 (Δ~(12)-PGJ_3) Analogues and Related Compounds

K. C. Nicolaou; Kiran Kumar Pulukuri; Stephan Rigol; Philipp Heretsch; Ruocheng Yu; Charles I. Grove; Christopher R. H. Hale; Abdelatif ElMarrouni; Verena Fetz; Mark Broenstrup; Monette Aujay; Joseph Sandoval; Julia Gavrilyuk

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Synthesis and Biological Investigation of Δ~(12)-Prostaglandin J_3 (Δ~(12)-PGJ_3) Analogues and Related Compounds

机译：Δ〜（12）-前列腺素J_3（Δ〜（12）-PGJ_3）类似物及相关化合物的合成及生物学研究

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A series of Δ~(12)-Prostaglandin J_3 (Δ~(12)-PGJ_3) analogues and derivatives were synthesized employing an array of synthetic strategies developed specifically to render them readily available for biological investigations. The synthesized compounds were evaluated for their cytotoxicity against a number of cancer cell lines, revealing nanomolar potencies for a number of them against certain cancer cell lines. Four analogues (2, 11, 21, and 27) demonstrated inhibition of nuclear export through a covalent addition at Cys528 of the export receptor Crm1. One of these compounds (i.e., 11) is currently under evaluation as a potential drug candidate for the treatment of certain types of cancer. These studies culminated in useful and path-pointing structure-activity relationships (SARs) that provide guidance for further improvements in the biological/pharmacological profiles of compounds within this class.

机译：使用一系列专门开发的合成策略合成了一系列Δ〜（12）-前列腺素J_3（Δ〜（12）-PGJ_3）类似物和衍生物，以使其易于用于生物学研究。评估了合成化合物对多种癌细胞系的细胞毒性，揭示了它们对某些癌细胞系的纳摩尔效能。四个类似物（2、11、21和27）证明了通过在受体Cym528的Cys528上共价添加来抑制核输出。这些化合物中的一种（即11种）目前正在评估中，作为治疗某些类型癌症的潜在候选药物。这些研究最终形成了有用的和指向路径的结构-活性关系（SAR），为进一步改善该类别化合物的生物学/药理特性提供了指导。

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来源
《Journal of the American Chemical Society》 |2016年第20期|6550-6560|共11页
作者
K. C. Nicolaou; Kiran Kumar Pulukuri; Stephan Rigol; Philipp Heretsch; Ruocheng Yu; Charles I. Grove; Christopher R. H. Hale; Abdelatif ElMarrouni; Verena Fetz; Mark Broenstrup; Monette Aujay; Joseph Sandoval; Julia Gavrilyuk;
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作者单位

Department of Chemistry, BioSdence Research Collaborative, Rice University, 6100 Main Street, Houston, Texas 77005, United States;

Department of Chemistry, BioSdence Research Collaborative, Rice University, 6100 Main Street, Houston, Texas 77005, United States,Stemcentrx Inc., 450 East Jamie Court, South San Francisco, California 94080, United States;

Department of Chemistry, BioSdence Research Collaborative, Rice University, 6100 Main Street, Houston, Texas 77005, United States,Stemcentrx Inc., 450 East Jamie Court, South San Francisco, California 94080, United States;

Department of Chemistry, BioSdence Research Collaborative, Rice University, 6100 Main Street, Houston, Texas 77005, United States,Stemcentrx Inc., 450 East Jamie Court, South San Francisco, California 94080, United States;

Department of Chemistry, BioSdence Research Collaborative, Rice University, 6100 Main Street, Houston, Texas 77005, United States;

Department of Chemistry, BioSdence Research Collaborative, Rice University, 6100 Main Street, Houston, Texas 77005, United States;

Department of Chemistry, BioSdence Research Collaborative, Rice University, 6100 Main Street, Houston, Texas 77005, United States;

Department of Chemistry, BioSdence Research Collaborative, Rice University, 6100 Main Street, Houston, Texas 77005, United States;

Department of Chemical Biology, Helmholtz Centre for Infection Research, Inhoffenstrasse 7, 38124 Braunschweig, Germany;

Department of Chemical Biology, Helmholtz Centre for Infection Research, Inhoffenstrasse 7, 38124 Braunschweig, Germany;

Stemcentrx Inc., 450 East Jamie Court, South San Francisco, California 94080, United States;

Stemcentrx Inc., 450 East Jamie Court, South San Francisco, California 94080, United States;

Stemcentrx Inc., 450 East Jamie Court, South San Francisco, California 94080, United States;

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收录信息美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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入库时间 2022-08-18 03:08:46

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Synthesis and Biological Investigation of Δ~(12)-Prostaglandin J_3 (Δ~(12)-PGJ_3) Analogues and Related Compounds

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