A Unique Pharmacophore for Activation of the Nuclear Orphan Receptor Nur77 In vivo and In vitro
Date
2010-04Author
Liu, Jing-jing ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Zeng, Hui-ni
Zhang, Lian-ru ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Zhan, Yan-yan ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Chen, Yan ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Wang, Yuan ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Wang, Juan
Xiang, Shao-hua
Liu, Wen-jun
Wang, Wei-jia ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Chen, Hang-zi ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Shen, Yue-mao ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Su, Wen-jin ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Huang, Pei-qiang
黄培强
Zhang, Hong-kui
Wu, Qiao ( Sch Life Sci, Key Lab Minist Educ Cell Biol & Tumor Cell Engn)
Collections
- 化学化工-已发表论文 [14469]
Abstract
Nur77 is a steroid orphan receptor that plays a critical role in regulating proliferation, differentiation, and apoptosis, including acting as a switch for Bcl-2 function. We previously reported that the octaketide cytosporone B (Csn-B) is a natural agonist for Nur77. In this study, we synthesized a series of Csn-B analogues and performed a structure-activity analysis that suggested criteria for the development of a unique pharmacophore to activate Nur77. The components of the pharmacophore necessary for binding Nur77 included the benzene ring, the phenolic hydroxyl group, and the acyl chain of the Csn-B scaffold, whereas the key feature for activating the biological function of Nur77 was the ester group. Csn-B analogues that bound Nur77 tightly not only stimulated its transactivation activity but also initiated mitochondrial apoptosis by means of novel crosstalk between Nur77 and BRE, an antiapoptotic protein regulated at the transcriptional level. Notably, the derivative n-amyl 2-[3,5-dihydroxy-2-(1-nonanoyl)phenyl] acetate exhibited greater antitumor activity in vivo than its parent compounds, highlighting particular interest in this compound. Our findings describe a pathway for rational design of Csn-B-derived Nur77 agonists as a new class of potent and effective antitumor agents. Cancer Res; 70(9); 3628-37. (C) 2010 AACR.
Citation
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