CircSLC4A7 in resistant-cells-derived exosomes promotes docetaxel resistance via the miR-1205/MAPT axis in prostate cancer

IF 3.7 3区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

IUBMB Life Pub Date : 2024-09-12 DOI:10.1002/iub.2915

Anhua Lin, Junhe Li, Wenjing He

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引用次数: 0

Abstract

Prostate cancer (PCa) is a high-mortality cancer. Docetaxel (DCT) combined with second-generation anti-androgens is considered the golden standard therapy for PCa, whose application is limited for DCT resistance (DR). Therefore, exploring the mechanism of DR is of great importance. In this study, PCa cell lines of PC3 and DU145 were employed, and DR cells were constructed by treatment with graded DCT. CircSLC4A7, miR-1205, and microtubule-associated protein tau (MAPT) transfections were established. Cell counting kit-8 assay was performed to evaluate the cell activity and IC₅₀ of DCT. After being treated with DCT, DR was assessed by colony formation assay, flow cytometry analysis, and terminal transferase-mediated UTP nick end-labeling assay. Real-time quantitative PCR and western blotting analysis evaluated the expression levels of genes. The dual-luciferase reporter gene assay verified the miR-1205 binding sites with circSLC4A7 and MAPT. An animal experiment was performed to assess the tumor growth influenced by circSLC4A7. After conducting DR cells and isolated exosomes, we found that not only co-culture with DR cells but also treatment with DR cells' exosomes would promote the DR of normal cells. Moreover, circSLC4A7 was highly expressed in DR cells and their exosomes. CircSLC4A7 overexpression enhanced DR, represented as raised IC50 of DCT, increased colony formation, and decreased cell apoptosis after DCT treatment, while circSLC4A7 knockdown had the opposite effect. MiR-1205 was confirmed as a circSLC4A7-sponged miRNA and miR-1205 inhibitor reversed the effect of sh-circSLC4A7. MAPT was further identified as a target of miR-1205 and had a similar effect with circSLC4A7. The effect of circSLC4A7 on DR was also confirmed by xenograft experiments. Collectively, circSLC4A7 in resistant-cells-derived exosomes promotes DCT resistance of PCa via miR-1205/MAPT axis, which may provide a new treatment strategy for DR of PCa.

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前列腺癌耐药细胞外泌体中的 CircSLC4A7 通过 miR-1205/MAPT 轴促进多西他赛耐药性的产生

前列腺癌（PCa）是一种死亡率很高的癌症。多西他赛（DCT）联合第二代抗雄激素被认为是治疗前列腺癌的黄金标准疗法，但DCT耐药（DR）限制了该疗法的应用。因此，探索DR的机制非常重要。本研究采用 PC3 和 DU145 PCa 细胞系，通过分级 DCT 处理构建 DR 细胞。转染CircSLC4A7、miR-1205和微管相关蛋白tau（MAPT）。进行细胞计数试剂盒-8测定以评估细胞活性和DCT的IC50。经 DCT 处理后，通过集落形成试验、流式细胞术分析和末端转移酶介导的UTP缺口末端标记试验评估 DR。实时定量 PCR 和 Western 印迹分析评估了基因的表达水平。双荧光素酶报告基因检测验证了 miR-1205 与 circSLC4A7 和 MAPT 的结合位点。为了评估 circSLC4A7 对肿瘤生长的影响，我们进行了动物实验。在对DR细胞和分离的外泌体进行实验后，我们发现不仅与DR细胞共培养，用DR细胞的外泌体处理也会促进正常细胞的DR。此外，circSLC4A7在DR细胞及其外泌体中高度表达。circSLC4A7过表达可增强DR，表现为DCT的IC50升高、集落形成增加以及DCT处理后细胞凋亡减少，而circSLC4A7敲除则有相反的效果。MiR-1205被证实是一种sponged miRNA，miR-1205抑制剂逆转了sh-circSLC4A7的作用。MAPT 被进一步确认为 miR-1205 的靶标，并与 circSLC4A7 有类似的作用。异种移植实验也证实了 circSLC4A7 对 DR 的影响。总之，耐药细胞外泌体中的circSLC4A7通过miR-1205/MAPT轴促进了PCa的DCT耐药，这可能为PCa的DR提供了一种新的治疗策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

IUBMB Life 生物-生化与分子生物学

CiteScore

10.60

自引率

0.00%

发文量

109

审稿时长

4-8 weeks

期刊介绍： IUBMB Life is the flagship journal of the International Union of Biochemistry and Molecular Biology and is devoted to the rapid publication of the most novel and significant original research articles, reviews, and hypotheses in the broadly defined fields of biochemistry, molecular biology, cell biology, and molecular medicine.