Src inhibition modulates AMBRA1-mediated mitophagy to counteract endothelial-to-mesenchymal transition in renal allograft fibrosis

IF 5.9 1区 生物学 Q2 CELL BIOLOGY Cell Proliferation Pub Date : 2024-06-29 DOI:10.1111/cpr.13699
Zeping Gui, Xuzhong Liu, Zhen Xu, Dengyuan Feng, Zhou Hang, Ming Zheng, Hao Chen, Shuang Fei, Li Sun, Jun Tao, Zhijian Han, Xiaobin Ju, Min Gu, Ruoyun Tan, Zijie Wang
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Abstract

Chronic allograft dysfunction (CAD) poses a significant challenge in kidney transplantation, with renal vascular endothelial-to-mesenchymal transition (EndMT) playing a vital role. While renal vascular EndMT has been verified as an important contributing factor to renal allograft interstitial fibrosis/tubular atrophy in CAD patients, its underlying mechanisms remain obscure. Currently, Src activation is closely linked to organ fibrosis development. Single-cell transcriptomic analysis in clinical patients revealed that Src is a potential pivotal mediator in CAD progression. Our findings revealed a significant upregulation of Src which closely associated with EndMT in CAD patients, allogeneic kidney transplanted rats and endothelial cells lines. In vivo, Src inhibition remarkably alleviate EndMT and renal allograft interstitial fibrosis in allogeneic kidney transplanted rats. It also had a similar antifibrotic effect in two endothelial cell lines. Mechanistically, the knockout of Src resulted in an augmented AMBRA1-mediated mitophagy in endothelial cells. We demonstrate that Src knockdown upregulates AMBRA1 level and activates mitophagy by stabilizing Parkin's ubiquitination levels and mitochondrial translocation. Subsequent experiments demonstrated that the knockdown of the Parkin gene inhibited mitophagy in endothelial cells, leading to increased production of Interleukin-6, thereby inducing EndMT. Consequently, our study underscores Src as a critical mediator of renal vascular EndMT and allograft interstitial fibrosis, exerting its impact through the regulation of AMBRA1/Parkin-mediated mitophagy.

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抑制 Src 可调节 AMBRA1 介导的有丝分裂,从而抵消肾脏异体移植纤维化过程中的内皮细胞向间质转化。
慢性移植物功能障碍(CAD)是肾移植的一大挑战,其中肾血管内皮细胞向间质转化(EndMT)起着至关重要的作用。虽然肾血管内皮细胞向间质转化(EndMT)已被证实是导致肾移植间质纤维化/肾小管萎缩的重要因素,但其潜在机制仍不清楚。目前,Src 激活与器官纤维化的发展密切相关。临床患者的单细胞转录组分析表明,Src 是导致 CAD 进展的潜在关键介质。我们的研究结果表明,在 CAD 患者、同种异体肾移植大鼠和内皮细胞系中,Src 的显著上调与 EndMT 密切相关。在体内,抑制 Src 能明显减轻同种异体肾移植大鼠的 EndMT 和肾移植间质纤维化。在两种内皮细胞系中也有类似的抗纤维化作用。从机理上讲,敲除 Src 会增强内皮细胞中 AMBRA1 介导的有丝分裂。我们证明,敲除 Src 会上调 AMBRA1 的水平,并通过稳定 Parkin 的泛素化水平和线粒体转运激活有丝分裂。随后的实验证明,Parkin 基因敲除抑制了内皮细胞的有丝分裂,导致白细胞介素-6 的产生增加,从而诱导内膜增生。因此,我们的研究强调了 Src 是肾脏血管内膜移植和移植物间质纤维化的关键介质,它通过调节 AMBRA1/Parkin 介导的有丝分裂产生影响。
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来源期刊
Cell Proliferation
Cell Proliferation 生物-细胞生物学
CiteScore
14.80
自引率
2.40%
发文量
198
审稿时长
1 months
期刊介绍: Cell Proliferation Focus: Devoted to studies into all aspects of cell proliferation and differentiation. Covers normal and abnormal states. Explores control systems and mechanisms at various levels: inter- and intracellular, molecular, and genetic. Investigates modification by and interactions with chemical and physical agents. Includes mathematical modeling and the development of new techniques. Publication Content: Original research papers Invited review articles Book reviews Letters commenting on previously published papers and/or topics of general interest By organizing the information in this manner, readers can quickly grasp the scope, focus, and publication content of Cell Proliferation.
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