In silico and functional analysis identifies key gene networks and novel gene candidates in obesity-linked human visceral fat

IF 4.2 2区 医学 Q1 ENDOCRINOLOGY & METABOLISM Obesity Pub Date : 2024-11-05 DOI:10.1002/oby.24161
Lijin Wang, Pratap Veerabrahma Seshachalam, Ruiming Chua, Hongwen Zhou, Sun Lei, Sujoy Ghosh
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Abstract

Objective

Visceral adiposity is associated with increased proinflammatory activity, insulin resistance, diabetes risk, and mortality rate. Numerous individual genes have been associated with obesity, but studies investigating gene regulatory networks in human visceral obesity have been lacking.

Methods

We analyzed gene regulatory networks in human visceral adipose tissue (VAT) from 48 and 11 Chinese patients with and without obesity, respectively, using gene coexpression and gene regulatory network construction from RNA-sequencing data. We also conducted RNA interference-based functional tests on selected genes for effects on adipocyte differentiation.

Results

A scale-free gene coexpression network was constructed from 360 differentially expressed genes between VAT samples from patients with and without obesity (absolute log fold change > 1, false discovery rate [FDR] < 0.05), with edge probability > 0.8. Gene regulatory network analysis identified candidate transcription factors associated with differentially expressed genes. A total of 15 subnetworks (communities) displayed altered connectivity patterns between obesity and nonobesity networks. Genes in proinflammatory pathways showed increased network connectivity in VAT samples with obesity, whereas the oxidative phosphorylation pathway displayed reduced connectivity (enrichment FDR < 0.05). Functional screening via RNA interference identified genes such as SOX30, SIRPB1, and OSBPL3 as potential network-derived candidates influencing adipocyte differentiation.

Conclusions

This approach highlights the network architecture in human obesity, identifies novel candidate genes, and generates new hypotheses regarding network-assisted gene regulation in VAT.

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硅学和功能分析确定了与肥胖相关的人类内脏脂肪中的关键基因网络和新型候选基因。
目的:内脏肥胖与促炎活动、胰岛素抵抗、糖尿病风险和死亡率增加有关。许多单个基因与肥胖有关,但缺乏对人类内脏肥胖基因调控网络的研究:方法:我们利用基因共表达和基因调控网络构建 RNA 序列数据,分析了分别来自 48 名和 11 名中国肥胖症和非肥胖症患者的内脏脂肪组织(VAT)的基因调控网络。我们还对选定基因进行了基于 RNA 干扰的功能测试,以确定其对脂肪细胞分化的影响:结果:我们从肥胖患者和非肥胖患者 VAT 样本的 360 个差异表达基因中构建了一个无标度基因共表达网络(绝对对折变化>1,假发现率 [FDR] 0.8)。基因调控网络分析确定了与差异表达基因相关的候选转录因子。共有 15 个子网络(群落)显示肥胖与非肥胖网络之间的连接模式发生了改变。在患有肥胖症的 VAT 样本中,促炎通路中的基因显示出更高的网络连通性,而氧化磷酸化通路则显示出更低的连通性(富集 FDR 结论):这种方法突出了人类肥胖症的网络结构,发现了新的候选基因,并提出了有关网络辅助调控 VAT 基因的新假设。
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来源期刊
Obesity
Obesity 医学-内分泌学与代谢
CiteScore
11.70
自引率
1.40%
发文量
261
审稿时长
2-4 weeks
期刊介绍: Obesity is the official journal of The Obesity Society and is the premier source of information for increasing knowledge, fostering translational research from basic to population science, and promoting better treatment for people with obesity. Obesity publishes important peer-reviewed research and cutting-edge reviews, commentaries, and public health and medical developments.
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Issue Information Poster Abstracts Oral Abstracts Issue Information Cardiometabolic characteristics of weight cycling: results from a mid-South regional comprehensive health care system
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