Hong Xu, Shujun Zeng, Yingmei Wang, Tong Yang, Minmin Wang, Xuan Li, Yejun He, Xin Peng, Xia Li, Qing Qiao, Jing Zhang
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Abstract
Therapeutic resistance is a notable cause of death in patients with ovarian carcinoma. Polyploid giant cancer cells (PGCCs), commonly arising in tumor tissues following chemotherapy, have recently been considered to contribute to drug resistance. As a type III deacetylase, Sirtuin1 (SIRT1) plays essential roles in the cell cycle, cellular senescence, and drug resistance. Accumulating evidence has suggested that alteration in its subcellular localization via nucleocytoplasmic shuttling is a critical process influencing the functions of SIRT1. However, the roles of SIRT1 subcellular localization in PGCC formation and subsequent senescence escape remain unclear. In this study, we compared the differences in the polyploid cell population and senescence state of PGCCs following paclitaxel treatment between tumor cells overexpressing wild-type SIRT1 (WT SIRT1) and those expressing nuclear localization sequence (NLS)-mutated SIRT1 (SIRT1NLSmt ). We investigated the involvement of cytoplasmic SIRT1 in biological processes and signaling pathways, including the cell cycle and cellular senescence, in ovarian carcinoma cells' response to paclitaxel treatment. We found that the SIRT1NLSmt tumor cell population contained more polyploid cells and fewer senescent PGCCs than the SIRT1-overexpressing tumor cell population. Comparative proteomic analyses using co-immunoprecipitation (Co-IP) combined with liquid chromatography–mass spectrometry (LC-MS)/MS showed the differences in the differentially expressed proteins related to PGCC formation, cell growth, and death, including CDK1 and CDK2, between SIRT1NLSmt and SIRT1 cells or PGCCs. Our results suggested that ovarian carcinoma cells utilize polyploidy formation as a survival mechanism during exposure to paclitaxel-based treatment via the effect of cytoplasmic SIRT1 on PGCC formation and survival, thereby boosting paclitaxel resistance. © 2023 The Pathological Society of Great Britain and Ireland.
细胞质SIRT1通过增加多倍体巨型癌细胞的形成和存活,促进卵巢癌紫杉醇耐药
治疗耐药性是卵巢癌患者死亡的一个显著原因。多倍体癌症巨细胞(PGCC)通常出现在化疗后的肿瘤组织中,最近被认为会导致耐药性。Sirtuin1(SIRT1)作为一种III型脱乙酰酶,在细胞周期、细胞衰老和耐药性中发挥着重要作用。越来越多的证据表明,通过核质穿梭改变其亚细胞定位是影响SIRT1功能的关键过程。然而,SIRT1亚细胞定位在PGCC形成和随后的衰老逃逸中的作用尚不清楚。在本研究中,我们比较了过表达野生型SIRT1(WT SIRT1)和表达核定位序列(NLS)突变SIRT1(SIRT1NLSmt)的肿瘤细胞在紫杉醇治疗后PGCC的多倍体细胞群和衰老状态的差异。我们研究了细胞质SIRT1在卵巢癌细胞对紫杉醇治疗反应的生物学过程和信号通路中的作用,包括细胞周期和细胞衰老。我们发现SIRT1NLSmt肿瘤细胞群体比SIRT1过表达的肿瘤细胞群体含有更多的多倍体细胞和更少的衰老PGCC。使用免疫共沉淀(co-IP)结合液相色谱-质谱(LC-MS)/MS的比较蛋白质组学分析显示,SIRT1NLSmt和SIRT1细胞或PGCC之间与PGCC形成、细胞生长和死亡相关的差异表达蛋白(包括CDK1和CDK2)存在差异。我们的结果表明,卵巢癌细胞在暴露于基于紫杉醇的治疗期间,通过细胞质SIRT1对PGCC形成和存活的影响,利用多倍体形成作为生存机制,从而增强紫杉醇耐药性。©2023大不列颠及爱尔兰病理学会。
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