Hyperinsulinemia is a probable trigger for weight gain and hyperphagia in individuals with Prader-Willi syndrome.

IF 1.9 Q3 ENDOCRINOLOGY & METABOLISM
Obesity Science & Practice Pub Date : 2023-02-17 eCollection Date: 2023-08-01 DOI:10.1002/osp4.663
Frederick A Kweh, Carlos R Sulsona, Jennifer L Miller, Daniel J Driscoll
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引用次数: 0

Abstract

Objective: Prader-Willi syndrome (PWS) is the most frequently diagnosed genetic cause of early childhood obesity. Individuals with PWS typically progress through 7 different nutritional phases during their lifetime. The main objective of this study was to assess potential factors, particularly insulin, that may be responsible for the weight gains in sub-phase 2a and their role in the subsequent increase in fat mass and obesity in sub-phase 2b and insatiable appetite in phase 3.

Methods: Fasting plasma insulin levels were measured in children with PWS between the ages of 0-12 years and in age-matched non-PWS participants with early-onset major (clinically severe) obesity (EMO) and in healthy-weight sibling controls (SC).

Results: Participants with PWS in nutritional phases 1a and 1b had plasma insulin levels comparable to SC. However, the transition from phase 1b up to phase 3 in the PWS group was accompanied by significant increases in insulin, coinciding in weight gains, obesity, and hyperphagia. Only individuals with PWS in phase 3 had comparable insulin levels to the EMO group who were higher than the SC group at any age.

Conclusions: Elevated insulin signaling is a probable trigger for weight gain and onset of hyperphagia in children with Prader-Willi syndrome. Regulating insulin levels early in childhood before the onset of the early weight gain may be key in modulating the onset and severity of obesity and hyperphagia in individuals with PWS, as well as in other young children with non-PWS early-onset obesity. Preventing or reversing elevated insulin levels in PWS with pharmacological agents and/or through diet restrictions such as a combined low carbohydrate, low glycemic-load diet may be a viable therapeutic strategy in combating obesity in children with PWS and others with early childhood obesity.

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高胰岛素血症可能是普拉德-威利综合征患者体重增加和食欲亢进的诱因。
目的:普拉德-威利综合征(PWS)是导致儿童早期肥胖最常见的遗传病因。PWS患者一生中通常会经历7个不同的营养阶段。本研究的主要目的是评估可能导致第 2a 亚阶段体重增加的潜在因素,尤其是胰岛素,以及它们在随后的第 2b 亚阶段脂肪量增加和肥胖以及第 3 阶段贪得无厌的食欲中的作用:方法:对0-12岁患有PWS的儿童、与年龄相匹配的非PWS早期重度(临床严重)肥胖(EMO)患者以及健康体重的兄弟姐妹对照组(SC)的空腹血浆胰岛素水平进行了测量:结果:处于营养阶段 1a 和 1b 的 PWS 患者的血浆胰岛素水平与 SC 相当。然而,PWS 组从 1b 阶段过渡到 3 阶段时,胰岛素显著增加,同时体重增加、肥胖和多食。只有处于第3阶段的PWS患者的胰岛素水平与EMO组相当,而EMO组的胰岛素水平在任何年龄都高于SC组:结论:胰岛素信号升高可能是普拉德-威利综合征患儿体重增加和食欲亢进的诱因。在儿童早期体重增加之前调节胰岛素水平可能是调节普氏综合征患儿以及其他非普氏综合征早发肥胖症幼儿肥胖症和吞食过多症发病和严重程度的关键。通过药物治疗和/或饮食限制(如低碳水化合物、低血糖负荷的综合饮食)来预防或逆转 PWS 患者胰岛素水平的升高,可能是防治 PWS 儿童和其他早期肥胖儿童肥胖症的可行治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Obesity Science & Practice
Obesity Science & Practice ENDOCRINOLOGY & METABOLISM-
CiteScore
4.20
自引率
4.50%
发文量
73
审稿时长
29 weeks
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