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第 3 外显子缺失的生长激素受体:在生理和病理条件下的分子和功能特征及其对 GH/IGF-I 轴的影响。

The exon 3-deleted growth hormone receptor: molecular and functional characterization and impact on GH/IGF-I axis in physiological and pathological conditions.

机构信息

Unit of Endocrinology and Diabetology, Department of Medical Sciences, Fondazione IRCCS Cà Granda Ospedale Maggiore Policlinico, University of Milan, Milan, Italy.

出版信息

J Endocrinol Invest. 2011 Dec;34(11):861-8. doi: 10.1007/BF03346731.

Abstract

The GH receptor (GHR) plays a key role in the the function of the GH/IGF-I axis and is the major effector of human growth. A common polymorphic variant consisting of genomic exon 3 deletion or retention (d3-GHR and full-length GHR, respectively), described in 2000, has been linked with increased receptor activity due to enhanced signal transduction. Subsequent pharmacogenetic studies have addressed a possible role of GHR polymorphism on the response to recombinant human GH treatment first in short children and then in adults, many of them suggesting that growth response to GH may be influenced, at least in some aspects, by this polymorphism. Similar studies, performed in patients with acromegaly, assumed an influence of the d3- GHR variant in the relationship between GH and IGF-I levels. More recently, some studies have investigated the relation between GHR genotype and treatment with the GHR antagonist pegvisomant, suggesting a better clinical response to therapy related to d3-GHR genotype. This review provides a summary of the main pharmacogenetic studies performed on this current and still open topic.

摘要

生长激素受体(GHR)在 GH/IGF-I 轴的功能中发挥着关键作用,是人类生长的主要效应器。2000 年描述的一种常见的多态性变异,由基因组外显子 3 的缺失或保留组成(分别为 d3-GHR 和全长 GHR),由于信号转导增强,与受体活性的增加有关。随后的药物遗传学研究探讨了 GHR 多态性对重组人生长激素治疗的反应的可能作用,首先是在身材矮小的儿童中,然后是在成年人中,其中许多研究表明,生长激素对生长的反应至少在某些方面可能受到这种多态性的影响。在肢端肥大症患者中进行的类似研究假设 d3-GHR 变体在 GH 和 IGF-I 水平之间的关系中起作用。最近,一些研究调查了 GHR 基因型与 GHR 拮抗剂培维索孟治疗之间的关系,表明与 d3-GHR 基因型相关的治疗有更好的临床反应。本综述总结了在这一当前且仍在开放的课题上进行的主要药物遗传学研究。

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