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脂肪组织巨噬细胞负担、全身炎症和胰岛素抵抗。

Adipose tissue macrophage burden, systemic inflammation, and insulin resistance.

机构信息

Endocrine Research Unit, Mayo Clinic, Rochester, Minnesota.

Department of Endocrinology and Metabolism, West China Hospital, Sichuan University, Chengdu, Sichuan, China.

出版信息

Am J Physiol Endocrinol Metab. 2020 Aug 1;319(2):E254-E264. doi: 10.1152/ajpendo.00109.2020. Epub 2020 Jun 2.

Abstract

Adipose tissue inflammation, as defined by macrophage accumulation, is proposed to cause insulin resistance and systemic inflammation. Because the strength of this relationship for humans is unclear, we tested whether adipose tissue macrophage (ATM) burden is correlated with these health indicators. Using immunohistochemistry, we measured abdominal subcutaneous CD68+ (total ATM), CD14+ (proinflammatory/M1), and CD206+ (anti-inflammatory/M2) ATM in 97 volunteers (BMI 20-38 kg/m, in addition to body composition, adipocyte size, homeostasis model assessment of insulin resistance, ADIPO-IR, adipose tissue insulin resistance measured by palmitate, plasma lipids, TNF, and IL-6 concentrations. There were several significant univariate correlations between metabolic parameters to IL-6 and ATM per 100 adipocytes, but not ATM per gram tissue; adipocyte size was a confounding variable. We used matching strategies and multivariate regression analyses to investigate the relationships between ATM and inflammatory/metabolic parameters independent of adipocyte size. Matching approaches revealed that the groups discordant for CD206 but concordant for adipocyte size had significantly different fasting insulin and IL-6 concentrations. However, groups discordant for adipocyte size but concordent for ATM differeded in that visceral fat, plasma triglyceride, glucose, and TNF concentrations were greater in those with large adipocytes. Multivariate regression analysis indicated that indexes of insulin resistance and fasting triglycerides were predicted by body composition; the predictive value of ATM per 100 adipocytes or per gram tissue was variable between males and females. We conclude that the relationship between ATM burden and metabolic/inflammatory variables is confounded by adipocyte size/body composition and that ATM do not predict insulin resistance, systemic inflammation, or dyslipidemia. ATM may primarily play a role in tissue remodeling rather than in metabolic pathology.

摘要

脂肪组织炎症,定义为巨噬细胞积累,被认为会导致胰岛素抵抗和全身炎症。由于这种关系在人类中的强度尚不清楚,我们测试了脂肪组织巨噬细胞(ATM)负担是否与这些健康指标相关。使用免疫组织化学,我们测量了 97 名志愿者腹部皮下的 CD68+(总 ATM)、CD14+(促炎/M1)和 CD206+(抗炎/M2)ATM(BMI 为 20-38 kg/m2),此外还有身体成分、脂肪细胞大小、胰岛素抵抗的稳态模型评估、ADIPO-IR、棕榈酸测量的脂肪组织胰岛素抵抗、血浆脂质、TNF 和 IL-6 浓度。代谢参数与 IL-6 和每 100 个脂肪细胞的 ATM 之间存在一些显著的单变量相关性,但与每克组织的 ATM 无关;脂肪细胞大小是一个混杂变量。我们使用匹配策略和多元回归分析来研究 ATM 与炎症/代谢参数之间的关系,这些关系独立于脂肪细胞大小。匹配方法表明,CD206 不一致但脂肪细胞大小一致的组之间的空腹胰岛素和 IL-6 浓度有显著差异。然而,脂肪细胞大小不一致但 ATM 一致的组之间存在差异,表现为大脂肪细胞的内脏脂肪、血浆甘油三酯、葡萄糖和 TNF 浓度更高。多元回归分析表明,胰岛素抵抗和空腹甘油三酯指数受身体成分预测;每 100 个脂肪细胞或每克组织的 ATM 的预测值在男性和女性之间是不同的。我们的结论是,ATM 负担与代谢/炎症变量之间的关系受到脂肪细胞大小/身体成分的混杂影响,并且 ATM 不能预测胰岛素抵抗、全身炎症或血脂异常。ATM 可能主要在组织重塑中发挥作用,而不是在代谢病理中发挥作用。

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