Mitotic stress-induced secretome primes cancer cells to apoptosis and maximizes paclitaxel response in breast tumors when combined with BCL-xL-targeting BH3 mimetics

有丝分裂应激诱导的分泌组可使癌细胞更容易凋亡,并且当与靶向 BCL-xL 的 BH3 模拟物联合使用时,可最大限度地提高乳腺肿瘤对紫杉醇的反应。

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作者:Lohard,Steven,Juin,Philippe P,Barillé-Nion,Sophie
期刊:Molecular and Cellular Oncology影响因子:1.900
时间:2020起止号:2020;7(3):1735912
doi:10.1080/23723556.2020.1735912研究方向: 肿瘤、表观遗传、细胞生物学

Abstract

We recently identified a previously unappreciated ability of antimitotics to propagate apoptotic priming across cancer cell populations. The underlying paracrine cytotoxic signal, fueled by undead cells activating the cGAS/STING pathway, is required for in vivo antitumor response and it can be further exploited by delayed, but not synchronous, BCL-xL inhibition.

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