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TSR2 高表达通过 PPAR 信号通路加重高血压。

Higher expression of TSR2 aggravating hypertension via the PPAR signaling pathway.

机构信息

Department of Cardiology, Beijing Tsinghua Changgung Hospital, School of Clinical Medicine, Tsinghua University, Beijing, China.

Department of Cardiology, Beijing Anzhen Hospital, Capital Medical University, National Clinical Research Center for Cardiovascular Diseases, Chaoyang 100029, Beijing, China.

出版信息

Aging (Albany NY). 2024 May 29;16(10):8980-8997. doi: 10.18632/aging.205852.

Abstract

Hypertension is a complex disease with unknown causes. Therefore, it's crucial to deeply study its molecular mechanism. The hypertension dataset was obtained from Gene Expression Omnibus data base (GEO), and miRNA regulating central hub genes was screened via weighted gene co-expression network (DEGs) and gene set enrichment (GSEA). Cell experiments validated TSR2's role and the PPAR signaling pathway through western blotting. 500 DEGs were identified for hypertension, mainly enriched in actin cross-linking, insulin signaling, PPAR signaling, and protein localization. Eight hub genes (SEC61G, SRP14, Liy AR, NIP7, SDAD1, POLR1D, DYNLL2, TSR2) were identified. Four hub genes (LYAR, SDAD1, POLR1D, TSR2) exhibited high expression levels in the hypertensive tissue samples, while showing low expression levels in the normal tissue samples. This led us to speculate that they may have relevant regulatory effects on hypertension. When TSR2 was knocked down in the hypertension peripheral blood mononuclear cells (PBMC) model, the critical proteins in the PPAR signaling pathway (FABP, PPAR, PLTP, ME1, SCD1, CYP27, FABP1, OLR1, CPT-1, PGAR, CAP, ADIPO, MMP1, UCP1, ILK, PDK1 UBC AQP7) were downregulated. This also occurred in the hypertension peripheral blood mononuclear cells (PBMC) + TSR2_ OV model. TSR2 is highly expressed in individuals with hypertension and may play a significant role in the development of hypertension through the PPAR signaling pathway. TSR2 could serve as a molecular target for the early diagnosis and precise treatment of hypertension, providing a valuable direction for the mechanism research of this condition.

摘要

高血压是一种病因不明的复杂疾病。因此,深入研究其分子机制至关重要。高血压数据集来自基因表达综合数据库(GEO),通过加权基因共表达网络(DEGs)和基因集富集分析(GSEA)筛选调节中枢基因的 miRNA。细胞实验通过 Western blot 验证了 TSR2 的作用和 PPAR 信号通路。确定了 500 个与高血压相关的 DEGs,主要富集在肌动蛋白交联、胰岛素信号、PPAR 信号和蛋白质定位。鉴定出 8 个 hub 基因(SEC61G、SRP14、LiyAR、NIP7、SDAD1、POLR1D、DYNLL2、TSR2)。四个 hub 基因(LYAR、SDAD1、POLR1D、TSR2)在高血压组织样本中表现出高表达水平,而在正常组织样本中表现出低表达水平。这让我们推测它们可能对高血压有相关的调节作用。在高血压外周血单核细胞(PBMC)模型中敲低 TSR2 时,PPAR 信号通路中的关键蛋白(FABP、PPAR、PLTP、ME1、SCD1、CYP27、FABP1、OLR1、CPT-1、PGAR、CAP、ADIPO、MMP1、UCP1、ILK、PDK1 UBC AQP7)下调。在高血压外周血单核细胞(PBMC)+TSR2_OV 模型中也发生了这种情况。TSR2 在高血压患者中高表达,可能通过 PPAR 信号通路在高血压的发生发展中发挥重要作用。TSR2 可以作为高血压早期诊断和精准治疗的分子靶点,为该疾病的机制研究提供有价值的方向。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4431/11164513/87abe4443a8e/aging-16-205852-g001.jpg

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