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White adipose tissue-infiltrated CD11b+ myeloid cells are a source of S100A4, a new potential marker of hepatic damage.
白色脂肪组织浸润的CD11b + 骨髓细胞是S100A4的来源,一种新的潜在的肝损伤标志物。
- 影响因子:5.04
- DOI:10.1530/EJE-20-1130
- 作者列表:"Reyes M","González L","Ibeas K","Cereijo R","Taxerås SD","Pellitero S","Martínez E","Tarascó J","Moreno P","Malagón P","Higueras C","Soria A","Puig-Domingo M","Villarroya F","Serra D","Herrero L","Sánchez-Infantes D
- 发表时间:2021-04-01
Abstract
Context:The endocrine and immunological properties of subcutaneous vs visceral adipose tissue (sWAT and vWAT, respectively) have turned a milestone in the study of metabolic diseases. The cytokine S100A4 is increased in obesity and has a role in adipose tissue dysfunction. However, the cellular source and its potential role in hepatic damage in obesity has not been elucidated. Objective:We aim to study the regulation of S100A4 in immune cells present in sWAT and vWAT, as well as its potential role as a circulating marker of hepatic inflammation and steatosis. Design:A cohort of 60 patients with obesity and distinct metabolic status was analyzed. CD11b+ myeloid cells and T cells were isolated from sWAT and vWAT by magnetic-activating cell sorting, and RNA was obtained. S100A4 gene expression was measured, and correlation analysis with clinical data was performed. Liver biopsies were obtained from 20 patients, and S100A4 circulating levels were measured to check the link with hepatic inflammation and steatosis. Results:S100A4 gene expression was strongly upregulated in sWAT- vs vWAT-infiltrated CD11b+ cells, but this modulation was not observed in T cells. S100A4 mRNA levels from sWAT (and not from vWAT) CD11b+ cells positively correlated with glycemia, triglycerides, TNF-α gene expression and proliferation markers. Finally, circulating S100A4 directly correlated with liver steatosis and hepatic inflammatory markers. Conclusion:Our data suggest that sWAT-infiltrated CD11b+ cells could be a major source of S100A4 in obesity. Moreover, our correlations identify circulating S100A4 as a potential novel biomarker of hepatic damage and steatosis.
摘要
背景: 皮下与内脏脂肪组织 (分别为sWAT和vWAT) 的内分泌和免疫学特性在代谢疾病的研究中成为里程碑。细胞因子S100A4在肥胖中增加并且在脂肪组织功能障碍中具有作用。然而,细胞来源及其在肥胖肝损伤中的潜在作用尚未阐明。 目的: 我们的目的是研究S100A4在存在于sWAT和vWAT的免疫细胞中的调节,以及其作为肝脏炎症和脂肪变性的循环标志物的潜在作用。 设计: 对60例肥胖和明显代谢状态患者进行队列分析。通过磁激活细胞分选从sWAT和vWAT分离CD11b + 髓样细胞和T细胞,并获得RNA。检测S100A4基因表达,并与临床资料进行相关性分析。从20名患者获得肝活检,并测量S100A4循环水平以检查与肝脏炎症和脂肪变性的联系。 结果: S100A4基因表达在sWAT- vs vWAT-浸润的CD11b + 细胞中强烈上调,但在T细胞中未观察到这种调节。来自sWAT (而不是来自vWAT) CD11b + 细胞的S100A4 mRNA水平与血糖、甘油三酯、TNF-α 基因表达和增殖标志物呈正相关。最后,循环S100A4与肝脏脂肪变性和肝脏炎症标志物直接相关。 结论: 我们的数据表明,sWAT浸润的CD11b + 细胞可能是肥胖中S100A4的主要来源。此外,我们的相关性确定了循环S100A4作为肝损伤和脂肪变性的潜在新型生物标志物。
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