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对伴糖尿病肾病的雄性和雌性 BTBR 小鼠的基因表达谱进行全面分析。

Comprehensive analysis of the gene expression profile of the male and female BTBR mice with diabetic nephropathy.

机构信息

Affiliated Mental Health Center & Hangzhou Seventh People's Hospital, Zhejiang University School of Medicine, Hangzhou, Zhejiang 310000, China.

Department of Pathogenic Biology, School of Basic Medical Science, Southwest Medical University, Luzhou, Sichuan 646000, China.

出版信息

Int J Biol Macromol. 2024 Feb;257(Pt 2):128720. doi: 10.1016/j.ijbiomac.2023.128720. Epub 2023 Dec 14.

Abstract

Comprehensive insight into the gender-based gene expression-related omics data in a rodent model of diabetic nephropathy (DN) is scarce. In the present study, the gender-based genes regulating different pathways involved in the progression of DN were explored through an unbiased RNA sequence of kidneys from BTBR mice with DN. We identified 17,739 and 17,981 genes in male and female DN mice; 1121 and 655 genes were expressed differentially (DEGs, differentially expressed genes) in male and female DN mice; both genders displayed only 195 DEGs. In the male DN mice, the number of upregulated genes was nearly the same as that of the down-regulated genes. In contrast, the number of upregulated genes was lesser than that of the down-regulated genes in the female DN mice, manifesting a remarkable gender disparity during the progression of DN in this animal model. Gene Ontology (GO) and KEGG-enriched results showed that most of these DEGs were related to the critical biological processes, including metabolic pathways, natural oxidation, bile secretion, and PPAR signaling; all are highly associated with DN. Notably, the DEGs significantly enriched for steroid hormone biosynthesis pathway were identified in both genders; the number of DEGs increased was 22 in male DN mice and 14 in female DN mice. Specifically, the Ugt1a10, Akr1c12, and Akr1c14 were upregulated in both genders. Interestingly, the Hsd11b1 gene was upregulated in female DN mice but downregulated in male DN mice. These results suggest that a significant gender-based variance in the gene expression occurs during the progression of DN and may be playing a role in the advancement of DN in the BTBR mouse model.

摘要

综合分析糖尿病肾病 (DN) 啮齿动物模型中基于性别的基因表达相关组学数据的研究甚少。本研究通过对 BTBR 糖尿病肾病小鼠肾脏进行无偏 RNA 测序,探索了调控不同通路的性别相关基因在 DN 进展中的作用。我们在雄性和雌性 DN 小鼠中分别鉴定到 17739 个和 17981 个基因;在雄性和雌性 DN 小鼠中分别有 1121 个和 655 个基因表达差异(DEGs,差异表达基因);两性中仅显示 195 个 DEGs。在雄性 DN 小鼠中,上调基因的数量几乎与下调基因的数量相同。相比之下,在雌性 DN 小鼠中,上调基因的数量少于下调基因的数量,在该动物模型中,DN 进展过程中存在显著的性别差异。GO 和 KEGG 富集结果表明,这些 DEGs 主要与包括代谢途径、天然氧化、胆汁分泌和 PPAR 信号转导在内的关键生物学过程相关,所有这些都与 DN 高度相关。值得注意的是,在两性中均鉴定到 DEGs 显著富集的甾体激素生物合成途径;雄性 DN 小鼠中 DEGs 的数量增加了 22 个,雌性 DN 小鼠中增加了 14 个。具体而言,Ugt1a10、Akr1c12 和 Akr1c14 在两性中均上调。有趣的是,Hsd11b1 基因在雌性 DN 小鼠中上调,而在雄性 DN 小鼠中下调。这些结果表明,在 DN 进展过程中存在显著的性别间基因表达差异,并且可能在 BTBR 小鼠模型中 DN 的进展中发挥作用。

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