SIRT4 protects against intestinal fibrosis by facilitating GLS1 degradation

IF 4.5 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Matrix Biology Pub Date : 2023-09-01 DOI:10.1016/j.matbio.2023.08.001
Xinru Xue , Xi Zeng , Xiaoqian Wu, Kexin Mu, Yue Dai, Zhifeng Wei
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Abstract

Intestinal fibrosis is a prevalent complication of Crohn's disease (CD), characterized by excessive deposition of extracellular matrix (ECM), and no approved drugs are currently available for its treatment. Sirtuin 4 (SIRT4), a potent anti-fibrosis factor in mitochondria, has an unclear role in intestinal fibrosis. In this study, fibroblasts isolated from biopsies of stenotic ileal mucosa in CD patients were analyzed to identify the most down-regulated protein among SIRT1–7, and SIRT4 was found to be the most affected. Moreover, in vivo and in vitro models of intestinal fibrosis, SIRT4 expression was significantly decreased in a TGF-β dependent manner, and its decrease was negatively associated with disease severity. SIRT4 impeded ECM deposition by inhibiting glutaminolysis, but not glycolysis, and α-ketoglutarate (α-KG) was identified as the key metabolite. Specifically, SIRT4 hinders SIRT5’s stabilizing interaction with glutaminase 1 (GLS1), thereby facilitating the degradation of GLS1. KDM6, rather than KDM4, is a potential mediator for α-KG-induced transcription of ECM components, and SIRT4 enhances the enrichment of H3K27me3 on their promotors and enhancers. These findings indicate that the activation of TGF-β signals decreases the expression of SIRT4 in intestinal fibrosis, and SIRT4 can facilitate GLS1 degradation, thereby resisting glutaminolysis and alleviating intestinal fibrosis, providing a novel therapeutic target for intestinal fibrosis.

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SIRT4通过促进GLS1降解来防止肠纤维化。
肠纤维化是克罗恩病(CD)的一种常见并发症,其特征是细胞外基质(ECM)过度沉积,目前尚无批准的药物可用于治疗。Sirtuin 4(SIRT4)是线粒体中一种有效的抗纤维化因子,在肠纤维化中的作用尚不清楚。在这项研究中,分析了从CD患者狭窄回肠粘膜活检中分离的成纤维细胞,以确定SIRT1-7中下调最多的蛋白,SIRT4受影响最大。此外,在肠纤维化的体内和体外模型中,SIRT4的表达以TGF-β依赖的方式显著降低,其降低与疾病严重程度呈负相关。SIRT4通过抑制谷氨酰胺分解而不是糖酵解来阻碍ECM沉积,α-酮戊二酸(α-KG)被确定为关键代谢产物。具体而言,SIRT4阻碍SIRT5与谷氨酰胺酶1(GLS1)的稳定相互作用,从而促进GLS1的降解。KDM6而不是KDM4是α-KG诱导的ECM成分转录的潜在介质,SIRT4增强了H3K27me3在其启动子和增强子上的富集。这些发现表明,TGF-β信号的激活降低了肠纤维化中SIRT4的表达,SIRT4可以促进GLS1的降解,从而抵抗谷氨酰胺分解,减轻肠纤维化,为肠纤维化提供了新的治疗靶点。
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来源期刊
Matrix Biology
Matrix Biology 生物-生化与分子生物学
CiteScore
11.40
自引率
4.30%
发文量
77
审稿时长
45 days
期刊介绍: Matrix Biology (established in 1980 as Collagen and Related Research) is a cutting-edge journal that is devoted to publishing the latest results in matrix biology research. We welcome articles that reside at the nexus of understanding the cellular and molecular pathophysiology of the extracellular matrix. Matrix Biology focusses on solving elusive questions, opening new avenues of thought and discovery, and challenging longstanding biological paradigms.
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