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Literature DB >> 25874343

Synthesis, molecular modeling, and biological evaluation of novel RAD51 inhibitors.

Jiewen Zhu¹, Hongyuan Chen¹, Xuning Emily Guo¹, Xiao-Long Qiu¹, Chun-Mei Hu², A Richard Chamberlin³, Wen-Hwa Lee⁴.

Abstract

RAD51 recombinase plays a critical role for cancer cell proliferation and survival. Targeting RAD51 is therefore an attractive strategy for treating difficult-to-treat cancers, e.g. triple negative breast cancers which are often resistant to existing therapeutics. To this end, we have designed, synthesized and evaluated a panel of new RAD51 inhibitors, denoted IBR compounds. Among these compounds, we have identified a novel small molecule RAD51 inhibitor, IBR120, which exhibited a 4.8-fold improved growth inhibition activity in triple negative human breast cancer cell line MBA-MD-468. IBR120 also inhibited the proliferation of a broad spectrum of other cancer cell types. Approximately 10-fold difference between the IC50 values in normal and cancer cells were observed. Moreover, IBR120 was capable of disrupting RAD51 multimerization, impairing homologous recombination repair, and inducing apoptotic cell death. Therefore, these novel RAD51 inhibitors may serve as potential candidates for the development of pharmaceutical strategies against difficult-to-treat cancers.

Entities: CellLine Chemical Disease Gene Species

Keywords: Breast cancer; Indole alkaloid; QSAR; RAD51 inhibitor; Synthesis; Triple-negative

Mesh：

Substances：

Year: 2015 PMID： 25874343 PMCID： PMC4433875 DOI： 10.1016/j.ejmech.2015.04.021

Source DB: PubMed Journal: Eur J Med Chem ISSN： 0223-5234 Impact factor: 6.514

22 in total

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