瘦素替代疗法治疗非haart相关脂肪营养不良综合征:瘦素对代谢和肝脏终点影响的荟萃分析

Alexander J Rodríguez, Teresa Neeman, Aaron G Giles, Claudio A Mastronardi, Gilberto Paz Filho
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引用次数: 19

摘要

脂质营养不良综合征(LS)的临床表现为高血糖、低脂血症、胰岛素抵抗、血脂异常和肝脂肪变性。瘦素替代疗法(LRT)对改善这些病理是有效的。目前,尚无数据汇编文献证据,证明LRT在LS患者中的作用。对MEDLINE和Cochrane图书馆数据库进行了系统回顾,以确定评估LRT对与高活性抗逆转录病毒治疗(HAART)使用无关的LS患者代谢和肝脏终点影响的研究。使用反方差随机效应模型,计算合并结果的标准化平均差异(SMD)和95%置信区间,以了解葡萄糖稳态、脂质谱和肝脏生理的总体变化。筛选后,纳入12项研究进行综述。226例患者的meta分析结果显示,LRT降低空腹血糖[0.75 SMD单位(范围0.36-1.13),p=0.0001],糖化血红蛋白[0.49 (0.17-0.81),p=0.003],甘油三酯[1.00 (0.69-1.31),p=0.0001]
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Leptin replacement therapy for the treatment of non-HAART associated lipodystrophy syndromes: a meta-analysis into the effects of leptin on metabolic and hepatic endpoints.

The clinical manifestations of lipodystrophy syndromes (LS) are hypoleptinemia, hyperglycemia, insulin resistance, dyslipidemia and hepatic steatosis. Leptin replacement therapy (LRT) is effective at improving these pathologies. Currently, there are no data compiling the evidence from the literature, and demonstrating the effect of LRT in LS patients. A systematic review of the MEDLINE and Cochrane Library databases was conducted to identify studies assessing the effect of LRT on metabolic and hepatic endpoints in patients with LS not associated with highly active antiretroviral therapy (HAART) use. Standardized mean differences (SMD) and 95% confidence intervals of pooled results were calculated for overall changes in glucose homeostasis, lipid profile, and hepatic physiology, using an inverse-variance random-effects model. After screening, 12 studies were included for review. Meta-analysis of results from 226 patients showed that LRT decreased fasting glucose [0.75 SMD units (range 0.36-1.13), p=0.0001], HbA1c [0.49 (0.17-0.81), p=0.003], triglycerides [1.00 (0.69-1.31), p<0.00001], total cholesterol [0.62 (0.21-1.02), p=0.003], liver volume [1.06 (0.51-1.61), p=0.0002] and AST [0.41 (0.10-0.73) p=0.01]. In patients with non-HAART LS, LRT improves the outcome of several metabolic and hepatic parameters. Studies were limited by small populations and therefore large prospective trials are needed to validate these findings.

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