Effects of growth hormone and pioglitazone in viscerally obese adults with impaired glucose tolerance: a factorial clinical trial.

PLoS clinical trials Pub Date : 2007-05-04 DOI:10.1371/journal.pctr.0020021

Hamdee Attallah, Anne L Friedlander, Matilde Nino-Murcia, Andrew R Hoffman

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引用次数: 15

Abstract

Objective: Recombinant human growth hormone (GH) and pioglitazone (PIO) in abdominally obese adults with impaired glucose tolerance were evaluated under the hypothesis that the combination attenuates GH-induced increases in glucose concentrations, reduces visceral adipose tissue (VAT), and improves insulin sensitivity over time.

Design: Randomized, double-blind, placebo-controlled, 2 x 2 factorial design.

Setting: Veterans Affairs Palo Alto Health Care System, Palo Alto, California, United States.

Participants: 62 abdominally obese adults aged 40-75 with impaired glucose tolerance.

Interventions: GH (8 microg/kg/d, or placebo) and pioglitazone (30 mg/d, or placebo) for 40 wk.

Outcome measures: Baseline and after 40 wk of treatment, VAT content was quantified by CT scan, glucose tolerance was assessed using a 75-g oral glucose tolerance test, and insulin sensitivity was measured using steady-state plasma glucose levels obtained during insulin suppression test.

Results: BASELINE: body mass index (BMI), plasma glucose, and visceral fat content were similar. 40 wk: visceral fat area declined 23.9 +/- 7.4 cm(2) in GH group, mean difference from placebo: -28.1 cm(2) (95% CI -49.9 to -6.3 cm(2); p = 0.02). Insulin resistance declined 52 +/- 11.8 mg/dl with PIO, mean difference from placebo of -58.8 mg/dl (95% CI -99.7 to -18.0 mg/dl; p = 0.01). VAT and SSPG declined with GH and PIO combined, mean differences from placebo of -31.4 cm(2) (95% CI -56.5 cm(2) to -6.3 cm(2); p = 0.02) and -55.3 mg/dl (95% CI -103.9 to -6.7 mg/dl; p = 0.02), respectively. Fasting plasma glucose increased transiently in GH group. No significant changes in BMI were observed.

Conclusions: Addition of PIO to GH attenuated the short-term diabetogenic effect of GH; the drug combination reduced VAT and insulin resistance over time. GH plus PIO may have added benefit on body composition and insulin sensitivity in the metabolic syndrome.

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生长激素和吡格列酮对糖耐量受损的内脏型肥胖成人的影响:一项析因临床试验。

目的：评估重组人生长激素（GH）和吡格列酮（PIO）在患有糖耐量受损的腹部肥胖成年人中的作用，假设这两种药物联合使用可以减轻GH诱导的葡萄糖浓度增加，减少内脏脂肪组织（VAT），并随时间提高胰岛素敏感性。设计：随机、双盲、安慰剂对照、2x2析因设计。背景：退伍军人事务部帕洛阿尔托医疗保健系统，美国加利福尼亚州帕洛阿尔特。参与者：62名40-75岁的腹部肥胖成年人，糖耐量受损。干预措施：生长激素（8微克/千克/天，或安慰剂）和吡格列酮（30毫克/天，安慰剂），持续40周。结果测量：基线和治疗40周后，通过CT扫描量化VAT含量，使用75-g口服葡萄糖耐量试验评估葡萄糖耐量，并使用胰岛素抑制试验中获得的稳态血糖水平测量胰岛素敏感性。结果：基线：体重指数（BMI）、血糖和内脏脂肪含量相似。40周：GH组内脏脂肪面积下降23.9+/-7.4 cm（2），与安慰剂组的平均差异：-28.1 cm（2；p=0.02）。PIO使胰岛素抵抗下降52+/-11.8 mg/dl，与安慰剂的平均差异为-58.8 mg/dl（95%CI-99.7至-18.0 mg/dl；p=0.01）。GH和PIO联合使用使VAT和SSPG下降，与安慰剂相比的平均差异是-31.4 cm（2）（95%CI-56.5 cm（2至-6.3 cm（2；p=0.02）和-55.3mg/dl（95%CI-103.9至-6.7mg/dl；p=0.02）。GH组空腹血糖瞬时升高。没有观察到BMI的显著变化。结论：在GH中加入PIO可减弱GH的短期致糖尿病作用；药物组合随着时间的推移降低了增值税和胰岛素抵抗。GH加PIO可能对代谢综合征的身体成分和胰岛素敏感性有额外的益处。

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