Cyclanoline Reverses Cisplatin Resistance in Bladder Cancer Cells by Inhibiting the JAK2/STAT3 Pathway.

IF 2.6 4区 医学 Q3 CHEMISTRY, MEDICINAL
Linjin Li, Chengpeng Li, Feilong Miao, Wu Chen, Xianghui Kong, Ruxian Ye, Feng Wang
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引用次数: 0

Abstract

Background: Cisplatin is a key therapeutic agent for bladder cancer, yet the emergence of cisplatin resistance presents a significant clinical challenge.

Objective: This study aims to investigate the potential and mechanisms of cyclanoline (Cyc) in overcoming cisplatin resistance.

Methods: Cisplatin-resistant T24 and BIU-87 cell models (T24/DR and BIU-87/DR) were established by increasing gradual concentration. Western Blot (WB) assessed the phosphorylation of STAT3, JAK2, and JAK3. T24/DR and BIU-87/DR cell lines were treated with selective STAT3 phosphorylation modulators, and cell viability was evaluated by CCK-8. Cells were subjected to cisplatin, Cyc, or their combination. Immunofluorescence (IHC) examined p-STAT3 expression. Protein and mRNA levels of apoptosis-related and cell cycle-related factors were measured. Changes in proliferation, invasion, migration, apoptosis, and cell cycle were monitored. In vivo, subcutaneous tumor transplantation models in nude mice were established, assessing tumor volume and weight. Changes in bladder cancer tissues were observed through HE staining, and the p-STAT3 was assessed via WB and IHC.

Results: Cisplatin-resistant cell lines were successfully established, demonstrating increased phosphorylation of STAT3, JAK2, and JAK3. Cisplatin or Cyc treatment decreased p-STAT3, inhibited invasion and migration, and induced apoptosis and cell cycle arrest in the G0/G1 phase in vitro. In vivo, tumor growth was significantly suppressed, with extensive tumor cell death. IHC and WB consistently showed a substantial downregulation of STAT3 phosphorylation. These changes were more pronounced when cisplatin and Cyc were administered in combination.

Conclusion: Cyc reverses cisplatin resistance via JAK/STAT3 inhibition in bladder cancer, offering a potential clinical strategy to enhance cisplatin efficacy in treating bladder cancer.

环甲唑啉通过抑制 JAK2/STAT3 通路逆转膀胱癌细胞的顺铂耐药性
背景:顺铂是治疗膀胱癌的主要药物,但顺铂耐药性的出现给临床带来了巨大挑战:顺铂是治疗膀胱癌的关键药物,但顺铂耐药性的出现给临床带来了巨大挑战:本研究旨在探讨环丙啉(Cyc)克服顺铂耐药性的潜力和机制:方法:通过逐渐增加浓度建立顺铂耐药的 T24 和 BIU-87 细胞模型(T24/DR 和 BIU-87/DR)。Western印迹(WB)评估STAT3、JAK2和JAK3的磷酸化。用选择性 STAT3 磷酸化调节剂处理 T24/DR 和 BIU-87/DR 细胞株,并用 CCK-8 评估细胞活力。细胞接受顺铂、Cyc或它们的组合治疗。免疫荧光(IHC)检测 p-STAT3 的表达。检测细胞凋亡相关因子和细胞周期相关因子的蛋白和 mRNA 水平。监测增殖、侵袭、迁移、凋亡和细胞周期的变化。建立裸鼠皮下肿瘤移植模型,评估肿瘤体积和重量。通过 HE 染色观察膀胱癌组织的变化,并通过 WB 和 IHC 评估 p-STAT3:结果:成功建立了顺铂耐药细胞系,表明 STAT3、JAK2 和 JAK3 磷酸化增加。顺铂或 Cyc 处理可降低 p-STAT3,抑制侵袭和迁移,并诱导细胞凋亡和细胞周期停滞在体外的 G0/G1 期。在体内,肿瘤生长明显受到抑制,肿瘤细胞大量死亡。IHC 和 WB 一致显示 STAT3 磷酸化水平大幅下调。这些变化在顺铂和 Cyc 联用时更为明显:结论:Cyc通过抑制膀胱癌中的JAK/STAT3逆转顺铂耐药性,为提高顺铂治疗膀胱癌的疗效提供了一种潜在的临床策略。
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来源期刊
Anti-cancer agents in medicinal chemistry
Anti-cancer agents in medicinal chemistry ONCOLOGY-CHEMISTRY, MEDICINAL
CiteScore
5.10
自引率
3.60%
发文量
323
审稿时长
4-8 weeks
期刊介绍: Formerly: Current Medicinal Chemistry - Anti-Cancer Agents. Anti-Cancer Agents in Medicinal Chemistry aims to cover all the latest and outstanding developments in medicinal chemistry and rational drug design for the discovery of anti-cancer agents. Each issue contains a series of timely in-depth reviews and guest edited issues written by leaders in the field covering a range of current topics in cancer medicinal chemistry. The journal only considers high quality research papers for publication. Anti-Cancer Agents in Medicinal Chemistry is an essential journal for every medicinal chemist who wishes to be kept informed and up-to-date with the latest and most important developments in cancer drug discovery.
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