Prader-Willi综合征小鼠模型中的瘦素信号缺陷:不再是孤儿遗传肥胖综合征?

Rare diseases (Austin, Tex.) Pub Date : 2013-03-27 eCollection Date: 2013-01-01 DOI:10.4161/rdis.24421
William F Colmers, Rachel Wevrick
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引用次数: 8

摘要

普瑞德-威利综合征(PWS)是一种罕见的遗传疾病(约1 / 12000),涉及染色体15q11-q13上至少6个基因。PWS患儿由于自愿活动减少、食物摄入增加,不仅体重迅速增加,严重肥胖,而且还表现为生长激素缺乏、白天嗜睡、内分泌失调和不孕。这些表型表明下丘脑功能障碍,下丘脑是调节短期和长期能量平衡和其他身体功能的大脑区域。PWS儿童肥胖的生理基础几十年来一直困扰着研究人员。Mercer等人现在证明,PWS基因之一的小鼠同源基因Magel2是下丘脑瘦素-黑素皮质素通路的一个组成部分,该通路对能量平衡至关重要。最有趣的是,该通路的其他成分的破坏会导致小鼠和人类的肥胖,这表明PWS与其他罕见的严重儿童期发病肥胖的遗传形式之间存在机制联系。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Leptin signaling defects in a mouse model of Prader-Willi syndrome: An orphan genetic obesity syndrome no more?

Leptin signaling defects in a mouse model of Prader-Willi syndrome: An orphan genetic obesity syndrome no more?

Prader-Willi syndrome (PWS) is a rare (~1 in 12,000) genetic disorder that involves at least six genes on chromosome 15q11-q13. Children with PWS not only rapidly gain weight and become severely obese because of reduced voluntary activity and increased food intake, but also exhibit growth hormone deficiency, excessive daytime sleepiness, endocrine dysregulation and infertility. These phenotypes suggest dysfunction of the hypothalamus, the brain region that regulates short- and long-term energy balance and other body functions. The physiological basis for obesity in children with PWS has eluded researchers for decades. Mercer et al. now demonstrate that Magel2, the murine ortholog of one of the PWS genes, is a component of the hypothalamic leptin-melanocortin pathway that is critical for energy balance. Most interestingly, disruptions of other components of this pathway cause obesity in both mice and humans, suggesting a mechanistic link between PWS and other rare genetic forms of severe childhood-onset obesity.

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