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生长激素信号缺陷分子诊断的当前问题

Current issues on molecular diagnosis of GH signaling defects.

作者信息

Feigerlova Eva, Hwa Vivian, Derr Michael A, Rosenfeld Ron G

机构信息

Department of Pediatrics, Oregon Health and Science University, Portland, Oreg., USA.

出版信息

Endocr Dev. 2013;24:118-27. doi: 10.1159/000342586. Epub 2013 Feb 1.

Abstract

The growth-promoting effects of GH are mediated primarily by regulating the biosynthesis of insulin-like growth factor (IGF)-1. The binding of circulating GH to the cell surface GH receptor (GHR) initiates signaling cascades, of which the signal transducer and activator of transcription (STAT)-5b pathway has proven, in both rodent models and human case studies, to be the most critical in regulating IGF-1 production. The identification of rare inactivating STAT5B mutations in children, whose severe postnatal growth retardation was associated with GH insensitivity (GHI) and IGF-1 deficiency, confirmed the importance of STAT5b in regulating IGF-1 gene expression. Unlike GHI due to mutations in the GHR gene, patients carrying STAT5B mutations often present with immune dysfunction that can lead to severe, life-threatening infections and chronic pulmonary disease, consistent with the fact that STAT5b is activated by multiple cytokines involved in immunity. The possibility of a STAT5b disorder should be considered, therefore, when children present with chronic infection and/or unexplained pulmonary disease concomitant with severe postnatal growth failure.

摘要

生长激素(GH)的促生长作用主要通过调节胰岛素样生长因子(IGF)-1的生物合成来介导。循环中的GH与细胞表面的GH受体(GHR)结合会启动信号级联反应,在啮齿动物模型和人类病例研究中均已证明,信号转导和转录激活因子(STAT)-5b途径在调节IGF-1产生方面最为关键。在儿童中发现罕见的STAT5B失活突变,其严重的出生后生长迟缓与GH不敏感(GHI)和IGF-1缺乏有关,这证实了STAT5b在调节IGF-1基因表达中的重要性。与因GHR基因突变导致的GHI不同,携带STAT5B突变的患者常出现免疫功能障碍,可导致严重的、危及生命的感染和慢性肺部疾病,这与STAT5b被多种参与免疫的细胞因子激活这一事实相符。因此,当儿童出现慢性感染和/或不明原因的肺部疾病并伴有严重的出生后生长衰竭时,应考虑STAT5b紊乱的可能性。

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