In vivo modulation of hypoxia-inducible signaling by topographical helix mimetics

被引:85
|
作者
Lao, Brooke Bullock [1 ]
Grishagin, Ivan [2 ]
Mesallati, Hanah [2 ]
Brewer, Thomas F. [1 ]
Olenyuk, Bogdan Z. [2 ]
Arora, Paramjit S. [1 ]
机构
[1] NYU, Dept Chem, New York, NY 10003 USA
[2] Univ So Calif, Sch Pharm, Dept Pharmacol & Pharmaceut Sci, Los Angeles, CA 90089 USA
基金
美国国家科学基金会;
关键词
helix mimics; hypoxia signaling; synthetic inhibitors of transcription; ENDOTHELIAL GROWTH-FACTOR; HIGH-HANGING FRUIT; PROTEIN INTERFACES; STRUCTURAL BASIS; INHIBITION; TRANSCRIPTION; CBP/P300; TARGETS; P300;
D O I
10.1073/pnas.1402393111
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Development of small-molecule inhibitors of protein-protein interactions is a fundamental challenge at the interface of chemistry and cancer biology. Successful methods for design of protein-protein interaction inhibitors include computational and experimental high-throughput and fragment-based screening strategies to locate small-molecule fragments that bind protein surfaces. An alternative rational design approach seeks to mimic the orientation and disposition of critical binding residues at protein interfaces. We describe the design, synthesis, biochemical, and in vivo evaluation of a small-molecule scaffold that captures the topography of a-helices. We designed mimics of a key a-helical domain at the interface of hypoxia-inducible factor 1 alpha and p300 to develop inhibitors of hypoxia-inducible signaling. The hypoxia-inducible factor/p300 interaction regulates the transcription of key genes, whose expression contributes to angiogenesis, metastasis, and altered energy metabolism in cancer. The designed compounds target the desired protein with high affinity and in a predetermined manner, with the optimal ligand providing effective reduction of tumor burden in experimental animal models.
引用
收藏
页码:7531 / 7536
页数:6
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