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接受治疗的HIV感染患者体内的促炎标志物、胰岛素敏感性和心脏代谢危险因素

Proinflammatory markers, insulin sensitivity, and cardiometabolic risk factors in treated HIV infection.

作者信息

Samaras Katherine, Gan Seng K, Peake Phillip W, Carr Andrew, Campbell Lesley V

机构信息

St Vincent's Hospital, Darlinghurst, New South Wales, Australia.

出版信息

Obesity (Silver Spring). 2009 Jan;17(1):53-9. doi: 10.1038/oby.2008.500. Epub 2008 Nov 13.

Abstract

Treated HIV infection and HIV-lipoatrophy increases risk of cardiovascular disease (CVD) and type 2 diabetes mellitus (T2DM). Circulating inflammatory molecules may, in part, explain this increased risk. This study examined circulating inflammatory molecules in treated HIV infection in relation to insulin sensitivity, lipids total body, and intramyocellular fat, compared to insulin-resistant obesity (an index group at high risk of diabetes). Detailed metabolic phenotypes were measured in 20 treated HIV-infected men (with and without subcutaneous lipoatrophy) vs. 26 insulin-resistant obese men (IR-O, n = 26), including inflammatory molecules, insulin sensitivity, total body fat (TBF), visceral fat (visceral adipose tissue (VAT)), and intramyocellular lipid (IMCL). C-reactive protein (CRP) levels in treated HIV were similar to those in IR-O, despite lower TBF and greater insulin sensitivity in treated HIV. In HIV-lipoatrophy, CRP was higher than that found in IR-O. Adiponectin was similar between treated HIV and IR-O, but significantly lower in those with HIV-lipoatrophy. In treated HIV, subjects with higher CRP had significantly higher total cholesterol, VAT, and IMCL. In treated HIV, subjects with lower adiponectin had significantly lower HDL and higher triglycerides, glucose, VAT, and IMCL. In conclusion, a proinflammatory milieu equivalent to that of insulin-resistant obesity characterizes lean men with treated HIV infection, worse in those with subcutaneous lipoatrophy. These factors may contribute to the accelerated diabetogenesis and cardiac risk observed in treated HIV infection.

摘要

接受治疗的HIV感染和HIV脂肪萎缩会增加心血管疾病(CVD)和2型糖尿病(T2DM)的风险。循环炎症分子可能在一定程度上解释了这种风险的增加。本研究检测了接受治疗的HIV感染者体内的循环炎症分子,并将其与胰岛素敏感性、全身脂质和肌内脂肪进行关联分析,同时与胰岛素抵抗性肥胖者(糖尿病高危指数组)进行比较。对20名接受治疗的HIV感染男性(有或无皮下脂肪萎缩)和26名胰岛素抵抗性肥胖男性(IR-O,n = 26)进行了详细的代谢表型检测,包括炎症分子、胰岛素敏感性、全身脂肪(TBF)、内脏脂肪(内脏脂肪组织(VAT))和肌内脂质(IMCL)。尽管接受治疗的HIV感染者TBF较低且胰岛素敏感性较高,但其C反应蛋白(CRP)水平与IR-O者相似。在HIV脂肪萎缩患者中,CRP高于IR-O者。接受治疗的HIV感染者与IR-O者的脂联素水平相似,但HIV脂肪萎缩患者的脂联素水平显著较低。在接受治疗的HIV感染者中,CRP较高的受试者总胆固醇、VAT和IMCL显著较高。在接受治疗的HIV感染者中,脂联素较低的受试者高密度脂蛋白显著较低,甘油三酯、血糖、VAT和IMCL较高。总之,接受治疗的HIV感染瘦男性存在与胰岛素抵抗性肥胖相当的促炎环境,皮下脂肪萎缩者情况更糟。这些因素可能导致接受治疗的HIV感染中观察到的糖尿病发病加速和心脏风险增加。

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