FUT8 upregulates CD36 and its core fucosylation to accelerate pericyte-myofibroblast transition through the mitochondrial-dependent apoptosis pathway during AKI-CKD.

IF 6 2区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Yaxi Shang, Ziran Wang, Fan Yang, Weidong Wang, Qingzhu Tang, Xianan Guo, Xiangning Du, Xu Zhang, Jiaojiao Hao, Hongli Lin
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引用次数: 0

Abstract

Background: Activation of pericytes leads to renal interstitial fibrosis, but the regulatory mechanism of pericytes in the progression from AKI to CKD remains poorly understood. CD36 activation plays a role in the progression of CKD. However, the significance of CD36 during AKI-CKD, especially in pericyte, remains to be fully defined.

Methods: GEO and DISCO database were used to analyze the expression of CD36 in pericyte during AKI-CKD; IRI to conduct AKI-CKD mouse model; Hypoxia/Reoxygenation (H/R) to induce the cell model; RT-qPCR and Western blotting to detect gene expression; IP and confocal-IF to determine the core fucosylation (CF) level of CD36. Flow cytometry (AV/PI staining) to detect the cell apoptosis and JC-1 staining to react to the change of mitochondrial membrane potential.

Results: During AKI to CKD progression, CD36 expression in pericytes is higher and may be influenced by CF. Moreover, we confirmed the positive association of CD36 expression with pericyte-myofibroblast transition and the progression of AKI-CKD in an IRI mouse model and hypoxia/reoxygenation (H/R) pericytes. Notably, we discovered that FUT8 upregulates both CD36 expression and its CF level, contributing to the activation of the mitochondrial-dependent apoptosis signaling pathway in pericytes, ultimately leading to the progression of AKI-CKD.

Conclusion: These results further identify FUT8 and CD36 as potential targets for the treatment in the progression of AKI-CKD.

在 AKI-CKD 期间,FUT8 上调 CD36 及其核心岩藻糖基化,通过线粒体依赖性凋亡途径加速周细胞-肌成纤维细胞转化。
背景:周细胞活化导致肾间质纤维化,但周细胞在从 AKI 进展到 CKD 过程中的调节机制仍不甚明了。CD36 的活化在 CKD 的进展中起着一定的作用。然而,CD36在AKI-CKD过程中的意义,尤其是在周细胞中的意义,仍有待完全明确:方法:利用 GEO 和 DISCO 数据库分析 AKI-CKD 期间 CD36 在周细胞中的表达;利用 IRI 建立 AKI-CKD 小鼠模型;利用低氧/再氧合(H/R)诱导细胞模型;利用 RT-qPCR 和 Western 印迹检测基因表达;利用 IP 和共聚焦-IF 测定 CD36 的核心岩藻糖基化(CF)水平。流式细胞术(AV/PI 染色)检测细胞凋亡,JC-1 染色反应线粒体膜电位的变化:结果:在 AKI 向 CKD 进展的过程中,周细胞中 CD36 的表达较高,可能受到 CF 的影响。此外,我们在 IRI 小鼠模型和低氧/复氧(H/R)周细胞中证实了 CD36 表达与周细胞-肌成纤维细胞转化和 AKI-CKD 进展的正相关。值得注意的是,我们发现 FUT8 可上调 CD36 的表达及其 CF 水平,有助于激活周细胞线粒体依赖性凋亡信号通路,最终导致 AKI-CKD 的进展:这些结果进一步确定了 FUT8 和 CD36 是治疗 AKI-CKD 进展的潜在靶点。
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来源期刊
Molecular Medicine
Molecular Medicine 医学-生化与分子生物学
CiteScore
8.60
自引率
0.00%
发文量
137
审稿时长
1 months
期刊介绍: Molecular Medicine is an open access journal that focuses on publishing recent findings related to disease pathogenesis at the molecular or physiological level. These insights can potentially contribute to the development of specific tools for disease diagnosis, treatment, or prevention. The journal considers manuscripts that present material pertinent to the genetic, molecular, or cellular underpinnings of critical physiological or disease processes. Submissions to Molecular Medicine are expected to elucidate the broader implications of the research findings for human disease and medicine in a manner that is accessible to a wide audience.
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