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内脏性肥胖、糖耐量受损、代谢综合征与生长激素治疗

Visceral obesity, impaired glucose tolerance, metabolic syndrome, and growth hormone therapy.

作者信息

Attallah Hamdee, Friedlander Anne L, Hoffman Andrew R

机构信息

Department of Medicine, Wayne State University, Detroit, MI, USA.

出版信息

Growth Horm IGF Res. 2006 Jul;16 Suppl A:S62-7. doi: 10.1016/j.ghir.2006.03.004. Epub 2006 Apr 18.

Abstract

Overweight adults with impaired glucose tolerance have a 5-10% risk of developing diabetes per year, and insulin resistance is an important cause of progression to diabetes in these individuals. Weight loss has been shown to improve insulin sensitivity and prevent or delay progression to diabetes. According to recent studies, the improvement in insulin sensitivity that occurs with weight loss is closely linked to the reduction of visceral adipose tissue (VAT), the collection of intra-abdominal adipose depots that includes omental and intrahepatic fat. After controlling for BMI, whole body fat, and subcutaneous fat, only VAT is an independent predictor of endogenous insulin sensitivity and glucose tolerance before or after weight loss. This, in turn, suggests that reducing VAT is crucial to improving insulin sensitivity and preventing diabetes in high-risk individuals. Recombinant human growth hormone (GH) is a lipolytic drug that reduces total body, abdominal, and visceral fat in growth hormone-deficient (GHD) adults. Several studies have reported substantial reductions in VAT following GH treatment in this population. Like GHD adults, abdominally obese individuals have increased VAT, insulin resistance, and growth hormone levels that are below normal during continuous 24-h monitoring. These similarities have prompted a number of recent investigations in abdominally obese adults that reported significant reductions in truncal and visceral fat and an improvement in insulin sensitivity following prolonged GH administration. However, other studies have shown that insulin resistance and glucose concentrations transiently worsen during the first few weeks of GH treatment and that these deleterious effects can persist even after VAT reduction has occurred. Prior studies involving GH treatment were generally limited to adults who were normoglycemic at baseline. Less is known about the effects of GH in adults with impaired glucose tolerance or diabetes. The effects of GH used in conjunction with insulin sensitizers on glycemic control and VAT in patients with impaired glucose tolerance will be reviewed.

摘要

糖耐量受损的超重成年人每年患糖尿病的风险为5%-10%,胰岛素抵抗是这些个体进展为糖尿病的重要原因。已证明体重减轻可改善胰岛素敏感性,并预防或延缓糖尿病的进展。根据最近的研究,体重减轻时发生的胰岛素敏感性改善与内脏脂肪组织(VAT)的减少密切相关,内脏脂肪组织是包括网膜和肝内脂肪在内的腹部脂肪堆积。在控制体重指数、全身脂肪和皮下脂肪后,只有VAT是体重减轻前后内源性胰岛素敏感性和糖耐量的独立预测指标。这反过来表明,减少VAT对于改善高危个体的胰岛素敏感性和预防糖尿病至关重要。重组人生长激素(GH)是一种促脂药物,可减少生长激素缺乏(GHD)成年人的全身、腹部和内脏脂肪。几项研究报告了该人群接受GH治疗后VAT的大幅减少。与GHD成年人一样,腹部肥胖个体的VAT增加、胰岛素抵抗增加,并且在连续24小时监测期间生长激素水平低于正常水平。这些相似之处促使最近对腹部肥胖成年人进行了一些研究,这些研究报告称,长期使用GH后,躯干和内脏脂肪显著减少,胰岛素敏感性得到改善。然而,其他研究表明,在GH治疗的最初几周内,胰岛素抵抗和血糖浓度会短暂恶化,即使在VAT减少后,这些有害影响仍可能持续。先前涉及GH治疗的研究通常仅限于基线血糖正常的成年人。关于GH对糖耐量受损或糖尿病成年人的影响知之甚少。本文将综述GH与胰岛素增敏剂联合使用对糖耐量受损患者血糖控制和VAT的影响。

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