先天免疫调节人类体内的脂肪因子。
Innate immunity modulates adipokines in humans.
作者信息
Anderson Paul D, Mehta Nehal N, Wolfe Megan L, Hinkle Christine C, Pruscino Leticia, Comiskey Lynne L, Tabita-Martinez Jennifer, Sellers Kimberly F, Rickels Michael R, Ahima Rexford S, Reilly Muredach P
机构信息
Cardiovascular Institute, University of Pennsylvania Medical Center, Philadelphia, PA 19104-6160, USA.
出版信息
J Clin Endocrinol Metab. 2007 Jun;92(6):2272-9. doi: 10.1210/jc.2006-2545. Epub 2007 Mar 20.
CONTEXT
Chronic inflammation converges in type 2 diabetes and atherosclerosis. Modulation of adipokine signaling by innate immunity in humans is of considerable interest given the role of adipokines in insulin resistance and atherosclerosis.
OBJECTIVE
The aim of the study was to examine effects of low-grade endotoxemia, a model of human inflammation, on adipokines in vivo.
DESIGN/SETTING: An open-label, placebo-controlled, fixed-sequence clinical study was conducted at a General Clinical Research Center.
PATIENTS
There were 20 healthy male (50%) and female volunteers aged 18-40 yr.
INTERVENTION
Serial blood sampling and adipose biopsies were performed for 24 h before and after iv bolus endotoxin [lipopolysaccharide (LPS), 3 ng/kg].
MAIN OUTCOME MEASURES
We measured plasma leptin, adiponectin, resistin, soluble leptin receptor, cytokines, insulin, and glucose; distribution of adiponectin among multimeric complexes; whole blood, monocyte and adipose mRNA for adipokines and their receptors.
RESULTS
LPS induced fever, blood, and adipose TNF and IL-6 and increased homeostasis model assessment of insulin resistance. These were associated with increases in plasma leptin (from 4.1 +/- 1.1 to 6.1 +/- 1.9 ng/ml in men; 21.1 +/- 4.4 to 27.4 +/- 4.7 ng/ml in women; P < 0.005), doubling of the leptin:soluble leptin receptor ratio, and marked induction of whole blood resistin mRNA (13.7 +/- 7.3-fold; P < 0.001) and plasma resistin (8.5 +/- 2.75 to 43.2 +/- 15.3 ng/ml; P < 0.001). Although total adiponectin levels and low and high molecular weight adiponectin complexes were unaltered by LPS treatment, whole blood mRNA for adiponectin receptors 1 (49%; P < 0.005) and 2 (65%; P < 0.001) was suppressed.
CONCLUSIONS
Modulation of adipokine signaling may contribute to the insulin resistant, atherogenic state associated with human inflammatory syndromes. Targeting of individual adipokines or their upstream regulation may prove effective in preventing acute and chronic inflammation-related metabolic complications.
背景
慢性炎症与2型糖尿病和动脉粥样硬化相关。鉴于脂肪因子在胰岛素抵抗和动脉粥样硬化中的作用,人类先天免疫对脂肪因子信号的调节备受关注。
目的
本研究旨在探讨人体炎症模型——低度内毒素血症对体内脂肪因子的影响。
设计/地点:在一个综合临床研究中心进行了一项开放标签、安慰剂对照、固定顺序的临床研究。
患者
有20名年龄在18 - 40岁的健康男性(50%)和女性志愿者。
干预
在静脉注射内毒素[脂多糖(LPS),3 ng/kg]前后24小时进行系列血液采样和脂肪组织活检。
主要观察指标
我们测量了血浆瘦素、脂联素、抵抗素、可溶性瘦素受体、细胞因子、胰岛素和葡萄糖;脂联素在多聚体复合物中的分布;脂肪因子及其受体的全血、单核细胞和脂肪组织mRNA。
结果
LPS引起发热、血液和脂肪组织中的肿瘤坏死因子(TNF)和白细胞介素-6(IL-6)升高,并增加了胰岛素抵抗的稳态模型评估值。这些变化与血浆瘦素升高有关(男性从4.1±1.1 ng/ml升至6.1±1.9 ng/ml;女性从21.1±4.4 ng/ml升至27.4±4.7 ng/ml;P<0.005),瘦素:可溶性瘦素受体比值翻倍,全血抵抗素mRNA显著诱导(13.7±7.3倍;P<0.001)以及血浆抵抗素升高(从8.5±2.75 ng/ml升至43.2±15.3 ng/ml;P<0.001)。虽然LPS处理未改变总脂联素水平以及低分子量和高分子量脂联素复合物,但脂联素受体1的全血mRNA(49%;P<0.005)和脂联素受体2的全血mRNA(65%;P<0.001)受到抑制。
结论
脂肪因子信号的调节可能导致与人类炎症综合征相关的胰岛素抵抗和动脉粥样硬化状态。针对单个脂肪因子或其上游调节进行干预可能对预防急性和慢性炎症相关的代谢并发症有效。
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