Small-molecule Bax agonists for cancer therapy

被引:0
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作者
Meiguo Xin
Rui Li
Maohua Xie
Dongkyoo Park
Taofeek K. Owonikoko
Gabriel L. Sica
Patrick E. Corsino
Jia Zhou
Chunyong Ding
Mark A. White
Andrew T. Magis
Suresh S. Ramalingam
Walter J. Curran
Fadlo R. Khuri
Xingming Deng
机构
[1] University of Florida,Department of Medicine
[2] Emory University School of Medicine and Winship Cancer Institute of Emory University,Department of Radiation Oncology
[3] Emory University School of Medicine and Winship Cancer Institute of Emory University,Department of Hematology and Medical Oncology
[4] Emory University School of Medicine and Winship Cancer Institute of Emory University,Department of Pathology
[5] University of Florida,Department of Pharmacology
[6] Chemical Biology Program,Department of Pharmacology and Toxicology
[7] University of Texas Medical Branch,undefined
[8] Sealy Center for Structural Biology and Molecular Biophysics,undefined
[9] University of Texas Medical Branch,undefined
[10] Institute for Systems Biology,undefined
[11] Present address: Xemabio LLC,undefined
[12] 4445 SW 35th Terrace Suite B,undefined
[13] Gainesville SW Industrial Park,undefined
[14] Gainesville,undefined
[15] Florida 32608,undefined
[16] USA.,undefined
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摘要
Bax, a central death regulator, is required at the decisional stage of apoptosis. We recently identified serine 184 (S184) of Bax as a critical functional switch controlling its proapoptotic activity. Here we used the structural pocket around S184 as a docking site to screen the NCI library of small molecules using the UCSF-DOCK programme suite. Three compounds, small-molecule Bax agonists SMBA1, SMBA2 and SMBA3, induce conformational changes in Bax by blocking S184 phosphorylation, facilitating Bax insertion into mitochondrial membranes and forming Bax oligomers. The latter leads to cytochrome c release and apoptosis in human lung cancer cells, which occurs in a Bax- but not Bak-dependent fashion. SMBA1 potently suppresses lung tumour growth via apoptosis by selectively activating Bax in vivo without significant normal tissue toxicity. Development of Bax agonists as a new class of anticancer drugs offers a strategy for the treatment of lung cancer and other Bax-expressing malignancies.
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