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下肢脂肪组织具有独特的发育特征,可抵抗肥胖相关代谢并发症。

Distinct developmental profile of lower-body adipose tissue defines resistance against obesity-associated metabolic complications.

机构信息

Oxford Centre for Diabetes, Endocrinology and Metabolism, University of Oxford, Oxford, U.K.

Department of Statistics, University of Oxford, Oxford, U.K. Medical Research Council Harwell, Harwell Science and Innovation Campus, Harwell, U.K.

出版信息

Diabetes. 2014 Nov;63(11):3785-97. doi: 10.2337/db14-0385. Epub 2014 Jun 19.

Abstract

Upper- and lower-body fat depots exhibit opposing associations with obesity-related metabolic disease. We defined the relationship between DEXA-quantified fat depots and diabetes/cardiovascular risk factors in a healthy population-based cohort (n = 3,399). Gynoid fat mass correlated negatively with insulin resistance after total fat mass adjustment, whereas the opposite was seen for abdominal fat. Paired transcriptomic analysis of gluteal subcutaneous adipose tissue (GSAT) and abdominal subcutaneous adipose tissue (ASAT) was performed across the BMI spectrum (n = 49; 21.4-45.5 kg/m(2)). In both depots, energy-generating metabolic genes were negatively associated and inflammatory genes were positively associated with obesity. However, associations were significantly weaker in GSAT. At the systemic level, arteriovenous release of the proinflammatory cytokine interleukin-6 (n = 34) was lower from GSAT than ASAT. Isolated preadipocytes retained a depot-specific transcriptional "memory" of embryonic developmental genes and exhibited differential promoter DNA methylation of selected genes (HOTAIR, TBX5) between GSAT and ASAT. Short hairpin RNA-mediated silencing identified TBX5 as a regulator of preadipocyte proliferation and adipogenic differentiation in ASAT. In conclusion, intrinsic differences in the expression of developmental genes in regional adipocytes provide a mechanistic basis for diversity in adipose tissue (AT) function. The less inflammatory nature of lower-body AT offers insight into the opposing metabolic disease risk associations between upper- and lower-body obesity.

摘要

身体上下部脂肪组织与肥胖相关代谢疾病呈相反关联。我们在一个基于人群的健康队列(n=3399)中定义了 DEXA 定量脂肪组织与糖尿病/心血管风险因素之间的关系。在调整总脂肪量后,女性型脂肪量与胰岛素抵抗呈负相关,而腹部脂肪则相反。对跨 BMI 谱(n=49;21.4-45.5kg/m2)的臀下皮下脂肪组织(GSAT)和腹部皮下脂肪组织(ASAT)进行了配对转录组分析。在两个部位,产生能量的代谢基因与肥胖呈负相关,而炎症基因与肥胖呈正相关。然而,在 GSAT 中,相关性明显较弱。在全身水平上,从 GSAT 释放的促炎细胞因子白细胞介素-6(n=34)低于 ASAT。分离的前体脂肪细胞保留了胚胎发育基因的特定部位转录“记忆”,并表现出 GSAT 和 ASAT 之间特定基因(HOTAIR、TBX5)的启动子 DNA 甲基化的差异。短发夹 RNA 介导的沉默鉴定出 TBX5 是 ASAT 中前体脂肪细胞增殖和脂肪生成分化的调节剂。总之,区域脂肪细胞中发育基因表达的内在差异为脂肪组织(AT)功能的多样性提供了机制基础。下半身 AT 的炎症反应性较低,为上半身和下半身肥胖与代谢疾病风险之间的相反关联提供了深入了解。

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