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发现一种有效的细胞毒剂,可促进恶性人咽鳞癌细胞系的 G/M 期细胞周期阻滞和细胞凋亡。

Discovery of a potent cytotoxic agent that promotes G/M phase cell cycle arrest and apoptosis in a malignant human pharyngeal squamous carcinoma cell line.

机构信息

Department of Basic and Translational Sciences, School of Dental Medicine, University of Pennsylvania, Philadelphia, PA 19104, USA.

出版信息

Int J Oncol. 2022 Apr;60(4). doi: 10.3892/ijo.2022.5331. Epub 2022 Feb 25.

DOI:10.3892/ijo.2022.5331
PMID:35211767
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8923654/
Abstract

Squamous cell carcinoma is the major form of malignancy that arises in head and neck cancer. The modest improvement in the 5‑year survival rate underpins its complex etiology and provides the impetus for the discovery of new therapeutics. The present study describes the discovery of an indole‑based small molecule (24a) that was a potent cytotoxic agent with antiproliferative and pro‑apoptotic properties against a pharyngeal carcinoma cell line, Detroit 562, effectively killing the cells at a half‑maximal inhibitory concentration of 0.03 µM, as demonstrated using cell proliferation studies. The antiproliferative property of 24a was demonstrated by its ability to promote G/M blockade, as assessed by cell cycle analysis using flow cytometry and the monitoring of real‑time cell cycle progression by the fluorescence ubiquitination‑based cell cycle indicator. This pro‑apoptotic property is supported by the promotion of TUNEL‑staining and increase in the activities of caspases‑3/7 and ‑6, in addition to the expression of death receptors and the cleavage of poly (ADP‑ribose) polymerase 1 protein as demonstrated by western blotting. Given that Detroit 562 lacks functional p53, it is suggested that 24a acts independently of the tumor suppressor.

摘要

鳞状细胞癌是头颈部癌症中主要的恶性肿瘤形式。5 年生存率的适度提高,说明了其复杂的病因,并为新疗法的发现提供了动力。本研究描述了一种吲哚为基础的小分子(24a)的发现,它是一种有效的细胞毒性剂,具有抗增殖和促凋亡特性,对咽癌细胞系 Detroit 562 有效,在半最大抑制浓度为 0.03 μM 时有效地杀死细胞,如细胞增殖研究所示。24a 的抗增殖特性通过其促进 G/M 阻断的能力来证明,通过使用流式细胞术进行细胞周期分析和监测实时细胞周期进展的荧光泛素化细胞周期指示剂来评估。这种促凋亡特性得到了 TUNEL 染色的促进以及 caspase-3/7 和 caspase-6 活性的增加的支持,此外,还通过 Western blot 证明了死亡受体的表达和聚(ADP-核糖)聚合酶 1 蛋白的切割。鉴于 Detroit 562 缺乏功能性 p53,因此 24a 被认为是独立于肿瘤抑制因子发挥作用的。

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