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阿霉素通过 PRMT5 介导的心肌成纤维细胞激活诱导小鼠心脏纤维化。

Adriamycin induces cardiac fibrosis in mice via PRMT5-mediated cardiac fibroblast activation.

机构信息

Wuxi School of Medicine, Jiangnan University, Wuxi, 214122, China.

School of Food Science and Technology, Jiangnan University, Wuxi, 214122, China.

出版信息

Acta Pharmacol Sin. 2023 Mar;44(3):573-583. doi: 10.1038/s41401-022-00963-x. Epub 2022 Sep 2.

DOI:10.1038/s41401-022-00963-x
PMID:36056082
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9958096/
Abstract

Long-term treatment with adriamycin (ADR) is associated with higher incidences of cumulative cardiotoxicity manifest as heart failure. ADR-induced cardiomyopathy is characterized by extensive fibrosis that is caused by cardiac fibroblast activation. To date, however, no specific treatment is available to alleviate ADR-induced cardiotoxicity. Protein arginine methyltransferase 5 (PRMT5), a major enzyme responsible for methylation of arginine, regulates numerous cellular processes such as cell differentiation. In the present study we investigated the role of PRMT5 in cardiac fibrosis. Mice were administered ADR (3 mg/kg, i.p., every 2 days) for 2 weeks. We showed that aberrant PRMT5 expression was largely co-localized with α-SMA-positive activated cardiac fibroblasts in ADR-injected mice and in ADR-treated cardiac fibroblasts in vitro. PRMT5-overexpression exacerbated, whereas PRMT5 knockdown alleviated ADR-induced cardiac fibrosis in vivo and TGF-β1-induced cardiac fibroblast activation in vitro. We demonstrated that PRMT5-overexpression enhanced methylated-Smad3 levels in vivo and in vitro. Pretreatment with a specific PRMT5 inhibitor EPZ015666 (5 nM) or overexpression of a catalytically inactive mutant of PRMT5, PRMT5(E444Q), reduced PRMT5-induced methylation of Smad3, thus suppressing PRMT5-mediated cardiac fibroblast activation in vitro. Furthermore, ADR activated cardiac fibroblasts was depending on autocrine TGF-β1. Taken together, our results demonstrate that PRMT5 promotes ADR-induced cardiac fibrosis via activating cardiac fibroblasts, suggesting that it may be a potential therapeutic target of ADR-caused cardiotoxicity.

摘要

长期使用阿霉素(ADR)会导致更高的累积性心脏毒性发生率,表现为心力衰竭。ADR 诱导的心肌病的特征是广泛的纤维化,这是由心脏成纤维细胞的激活引起的。然而,迄今为止,尚无特异性治疗方法可减轻 ADR 诱导的心脏毒性。蛋白精氨酸甲基转移酶 5(PRMT5)是一种主要负责精氨酸甲基化的酶,调节着细胞分化等许多细胞过程。在本研究中,我们研究了 PRMT5 在心脏纤维化中的作用。用 ADR(3mg/kg,腹腔注射,每 2 天一次)处理小鼠 2 周。我们表明,在 ADR 注射小鼠和 ADR 处理的心脏成纤维细胞中,异常的 PRMT5 表达与 α-SMA 阳性激活的心脏成纤维细胞大部分共定位。PRMT5 过表达加剧,而 PRMT5 敲低减轻了体内 ADR 诱导的心脏纤维化和体外 TGF-β1 诱导的心脏成纤维细胞激活。我们证明 PRMT5 过表达增强了体内和体外甲基化 Smad3 水平。用特异性 PRMT5 抑制剂 EPZ015666(5nM)预处理或过表达 PRMT5 的催化失活突变体 PRMT5(E444Q),降低了 PRMT5 诱导的 Smad3 甲基化,从而抑制了体外 PRMT5 介导的心脏成纤维细胞激活。此外,ADR 激活的心脏成纤维细胞依赖自分泌 TGF-β1。总之,我们的结果表明,PRMT5 通过激活心脏成纤维细胞促进 ADR 诱导的心脏纤维化,表明它可能是 ADR 引起的心脏毒性的潜在治疗靶点。

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