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Data from Modulation of Bax and mTOR for Cancer Therapeutics

Posted on 2023-03-31 - 00:46
Abstract

A rationale exists for pharmacologic manipulation of the serine (S)184 phosphorylation site of the proapoptotic Bcl2 family member Bax as an anticancer strategy. Here, we report the refinement of the Bax agonist SMBA1 to generate CYD-2-11, which has characteristics of a suitable clinical lead compound. CYD-2-11 targeted the structural pocket proximal to S184 in the C-terminal region of Bax, directly activating its proapoptotic activity by inducing a conformational change enabling formation of Bax homooligomers in mitochondrial membranes. In murine models of small-cell and non–small cell lung cancers, including patient-derived xenograft and the genetically engineered mutant KRAS-driven lung cancer models, CYD-2-11 suppressed malignant growth without evident significant toxicity to normal tissues. In lung cancer patients treated with mTOR inhibitor RAD001, we observed enhanced S184 Bax phosphorylation in lung cancer cells and tissues that inactivates the propaoptotic function of Bax, contributing to rapalog resistance. Combined treatment of CYD-2-11 and RAD001 in murine lung cancer models displayed strong synergistic activity and overcame rapalog resistance in vitro and in vivo. Taken together, our findings provide preclinical evidence for a pharmacologic combination of Bax activation and mTOR inhibition as a rational strategy to improve lung cancer treatment. Cancer Res; 77(11); 3001–12. ©2017 AACR.

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FUNDING

NIH

Gulf Coast Consortia

John Sealy Memorial Endowment Fund

Winship Research Pathology and Intergrated Cellular Imaging shared resource

Winship Cancer Institute of Emory University

Winship Fashion a Cure Research Scholar Award

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Cancer Research

AUTHORS (23)

  • Rui Li
    Chunyong Ding
    Jun Zhang
    Maohua Xie
    Dongkyoo Park
    Ye Ding
    Guo Chen
    Guojing Zhang
    Melissa Gilbert-Ross
    Wei Zhou
    Adam I. Marcus
    Shi-Yong Sun
    Zhuo G. Chen
    Gabriel L. Sica
    Suresh S. Ramalingam
    Andrew T. Magis
    Haian Fu
    Fadlo R. Khuri
    Walter J. Curran
    Taofeek K. Owonikoko
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