转录因子 TEAD4 对 CDC25B 的上调通过细胞粘附作用驱动胃腺癌的侵袭并抑制顺铂敏感性

IF 1.8 4区 医学 Q3 ONCOLOGY Anti-Cancer Drugs Pub Date : 2024-11-01 Epub Date: 2024-07-22 DOI:10.1097/CAD.0000000000001645
Tao Zhang, Lijian Chen, Shuang Li, Chao Shen
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引用次数: 0

摘要

顺铂是治疗晚期胃腺癌的关键,而化疗耐药性的产生会阻碍顺铂的整体疗效。本研究旨在探索 CDC25B 在胃腺癌顺铂敏感性中的作用,并为解释其功能提供一种可能的机制。通过生物信息学方法,分析了 CDC25B 和 TEAD4 在胃腺癌组织中的表达水平以及 CDC25B 的富集通路。细胞粘附实验检测了细胞的粘附能力。Western 印迹检测细胞粘附相关蛋白的表达,特别是 Muc-1、ICAM-1 和 VCAM-1。双荧光素酶实验和 ChIP 实验验证了 TEAD4 和 CDC25B 之间的结合关系。CDC25B 在胃腺癌组织和细胞中上调,富集于局灶粘附通路。用细胞粘附抑制剂处理发现,CDC25B过表达可通过细胞粘附途径抑制胃腺癌对顺铂的敏感性。CDC25B有一个上游转录因子TEAD4,TEAD4与CDC25B靶向结合,并在胃腺癌中高表达。拯救实验发现,敲除TEAD4可削弱CDC25B过表达对胃腺癌细胞顺铂敏感性的抑制作用。转录因子TEAD4可通过细胞粘附激活CDC25B的转录,从而驱动细胞侵袭并降低胃腺癌对顺铂的敏感性。TEAD4和CDC25B可能成为治疗胃腺癌的新靶点。
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Upregulation of CDC25B by transcription factor TEAD4 drives invasion and inhibits cisplatin sensitivity through cell adhesion in stomach adenocarcinoma.

Cisplatin is crucial in management of advanced stomach adenocarcinoma, whereas development of chemotherapy resistance hinders overall efficacy of cisplatin. This work aims to explore role of CDC25B in cisplatin sensitivity in stomach adenocarcinoma and offer a possible mechanism for explaining its function. By using bioinformatics approaches, CDC25B and TEAD4 expression levels in stomach adenocarcinoma tissues and enriched pathways of CDC25B were analyzed. qRT-PCR of CDC25B and TEAD4 expression in stomach adenocarcinoma cells, CCK-8 detection of cell viability and IC 50 values, and colony formation assay on cell proliferation were performed. Cell adhesion experiment detected cell adhesion ability. Western blot detected expression of proteins related to cell adhesion, specifically Muc-1, ICAM-1, VCAM-1. Dual luciferase assay and ChIP experiment verified binding relationship between TEAD4 and CDC25B. CDC25B was upregulated in stomach adenocarcinoma tissues and cells, enriched in focal adhesion pathway. Treatment with cell adhesion inhibitors revealed that CDC25B overexpression inhibits the sensitivity of stomach adenocarcinoma to cisplatin through the cell adhesion pathway. CDC25B has an upstream transcription factor TEAD4, which targeted and bound to CDC25B and was highly expressed in stomach adenocarcinoma. Rescue experiment revealed that knocking down TEAD4 weakened suppressive impact of CDC25B overexpression on sensitivity of stomach adenocarcinoma cells to cisplatin. Transcription factor TEAD4 could activate the transcription of CDC25B through cell adhesion to drive cell invasion and reduce sensitivity of stomach adenocarcinoma to cisplatin. TEAD4 and CDC25B may become new targets for management of stomach adenocarcinoma.

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来源期刊
Anti-Cancer Drugs
Anti-Cancer Drugs 医学-药学
CiteScore
3.80
自引率
0.00%
发文量
244
审稿时长
3 months
期刊介绍: Anti-Cancer Drugs reports both clinical and experimental results related to anti-cancer drugs, and welcomes contributions on anti-cancer drug design, drug delivery, pharmacology, hormonal and biological modalities and chemotherapy evaluation. An internationally refereed journal devoted to the fast publication of innovative investigations on therapeutic agents against cancer, Anti-Cancer Drugs aims to stimulate and report research on both toxic and non-toxic anti-cancer agents. Consequently, the scope on the journal will cover both conventional cytotoxic chemotherapy and hormonal or biological response modalities such as interleukins and immunotherapy. Submitted articles undergo a preliminary review by the editor. Some articles may be returned to authors without further consideration. Those being considered for publication will undergo further assessment and peer-review by the editors and those invited to do so from a reviewer pool.
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