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拉布森-门登霍尔综合征患者用 metreleptin 的长期疗效对血糖、生长和肾功能的影响。

Long-Term Effects of Metreleptin in Rabson-Mendenhall Syndrome on Glycemia, Growth, and Kidney Function.

机构信息

Diabetes, Endocrinology, and Obesity Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

J Clin Endocrinol Metab. 2022 Feb 17;107(3):e1032-e1046. doi: 10.1210/clinem/dgab782.

Abstract

CONTEXT

Rabson-Mendenhall syndrome (RMS) is caused by biallelic pathogenic variants in the insulin receptor gene (INSR) leading to insulin-resistant diabetes, microvascular complications, and growth hormone resistance with short stature. Small, uncontrolled studies suggest that 1-year treatment with recombinant leptin (metreleptin) improves glycemia in RMS.

OBJECTIVE

This study aimed to determine effects of long-term metreleptin in RMS on glycemia, anthropometrics, the growth hormone axis, and kidney function.

METHODS

We compared RMS patients during nonrandomized open-label treatment with metreleptin (≥ 0.15 mg/kg/day) vs no metreleptin over 90 months (5 subjects in both groups at different times, 4 only in metreleptin group, 2 only in control group). Main outcome measures were A1c; glucose; insulin; 24-hour urine glucose; standard deviation scores (SDS) for height, weight, body mass index (BMI), and insulin-like growth factor 1 (IGF-1); growth hormone; and estimated glomerular filtration rate.

RESULTS

Over time, metreleptin-treated subjects maintained 1.8 percentage point lower A1c vs controls (P = 0.007), which remained significant after accounting for changes in insulin doses. Metreleptin-treated subjects had a reduction in BMI SDS, which predicted decreased A1c. Growth hormone increased after metreleptin treatment vs control, with no difference in SDS between groups for IGF-1 or height. Reduced BMI predicted higher growth hormone, while reduced A1c predicted higher IGF-1.

CONCLUSION

Metreleptin alters the natural history of rising A1c in RMS, leading to lower A1c throughout long-term follow-up. Improved glycemia with metreleptin is likely attributable to appetite suppression and lower BMI SDS. Lower BMI after metreleptin may also worsen growth hormone resistance in RMS, resulting in a null effect on IGF-1 and growth despite improved glycemia.

摘要

背景

拉布森-门登霍尔综合征(RMS)是由胰岛素受体基因(INSR)的双等位致病性变异引起的,导致胰岛素抵抗性糖尿病、微血管并发症和生长激素抵抗导致身材矮小。小型、未对照的研究表明,1 年的重组瘦素(metreleptin)治疗可改善 RMS 的血糖水平。

目的

本研究旨在确定长期 metreleptin 在 RMS 中的血糖、人体测量学、生长激素轴和肾功能的影响。

方法

我们比较了 RMS 患者在 metreleptin(≥0.15mg/kg/天)治疗的非随机开放标签治疗期间与无 metreleptin 治疗期间的情况,共 90 个月(两组中不同时间各有 5 名患者,仅 metreleptin 组有 4 名患者,仅对照组有 2 名患者)。主要观察指标为 A1c;血糖;胰岛素;24 小时尿糖;身高、体重、体重指数(BMI)和胰岛素样生长因子 1(IGF-1)的标准差分数(SDS);生长激素;和估计的肾小球滤过率。

结果

随着时间的推移,metreleptin 治疗组的 A1c 比对照组低 1.8 个百分点(P=0.007),在考虑胰岛素剂量变化后仍有显著差异。Metreleptin 治疗组的 BMI SDS 降低,这预示着 A1c 降低。生长激素在 metreleptin 治疗后增加,而 IGF-1 或身高两组之间的 SDS 无差异。BMI 降低预示着生长激素升高,而 A1c 降低预示着 IGF-1 升高。

结论

Metreleptin 改变了 RMS 中 A1c 升高的自然史,导致长期随访中 A1c 降低。Metreleptin 改善血糖可能归因于食欲抑制和 BMI SDS 降低。尽管血糖改善,但 metreleptin 后 BMI 降低可能也会使 RMS 中的生长激素抵抗恶化,导致 IGF-1 和生长无明显变化。

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