中国科学院机构知识库网格
Chinese Academy of Sciences Institutional Repositories Grid
advancesinsmallmoleculegpr40agonistsfortreatmentoftype2diabetesmellitus

文献类型:期刊论文

作者Li H(李鹤); Long YQ(龙亚秋)
刊名chinesejournaloforganicchemistry
出版日期2016
卷号36期号:4页码:736
关键词1 FFA1/GPR40 AGONIST IN-VITRO DISCOVERY POTENT ACIDS IDENTIFICATION OPTIMIZATION CELLS type II diabetes mellitus GPR40 agonists glucose-stimulated insulin secretion phenylpropanoic acid
ISSN号0253-2786
DOI10.6023/cjoc201511011
英文摘要Currently, the majority of the chemotherapy for type 2 diabetes mellitus (T2DM) functions through glycemic control by administration of oral or injectable hypoglycemic drugs. Though a range of anti-diabetic drugs with different modes of action have been launched, there still remains a significant need for development of effective and highly safe anti-diabetic agents for the increasing diabetic population. GPR40 belongs to the GPCR family and the activation of GPR40 can amplify glucose-stimulated insulin secretion (GSIS). Due to the advantage of minimizing the hypoglycemia risk, GPR40 has drawn more and more attention and emerged as a promising new target for T2DM treatment. Therefore, the recent progress on the structural optimization and further development of small molecule GPR40 agonists as novel treatment for T2DM is reviewed, focused on those under clinical trials or at preclinical stage. A variety of small molecule GPR40 agonists were summarized from the literature and patents based on the pharmacophore model, including the critical phenylpropanoic acid core, the hydrophobic terminus and the linker. The structural features and advantage of different sources of GPR40 agonists were analyzed and highlighted.
资助项目[National Natural Science Foundation of China]
语种英语
源URL[http://119.78.100.183/handle/2S10ELR8/284171]  
专题中国科学院上海药物研究所
作者单位中国科学院上海药物研究所
推荐引用方式
GB/T 7714
Li H,Long YQ. advancesinsmallmoleculegpr40agonistsfortreatmentoftype2diabetesmellitus[J]. chinesejournaloforganicchemistry,2016,36(4):736.
APA 李鹤,&龙亚秋.(2016).advancesinsmallmoleculegpr40agonistsfortreatmentoftype2diabetesmellitus.chinesejournaloforganicchemistry,36(4),736.
MLA 李鹤,et al."advancesinsmallmoleculegpr40agonistsfortreatmentoftype2diabetesmellitus".chinesejournaloforganicchemistry 36.4(2016):736.

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来源:上海药物研究所

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