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永生化非洲俾格米人T细胞中胰岛素样生长因子I受体表达和功能降低。

Decreased insulin-like growth factor I receptor expression and function in immortalized African Pygmy T cells.

作者信息

Hattori Y, Vera J C, Rivas C I, Bersch N, Bailey R C, Geffner M E, Golde D W

机构信息

Program in Molecular Pharmacology and Therapeutics, Memorial Sloan-Kettering Cancer Center, New York, New York 10021, USA.

出版信息

J Clin Endocrinol Metab. 1996 Jun;81(6):2257-63. doi: 10.1210/jcem.81.6.8964861.

DOI:10.1210/jcem.81.6.8964861
PMID:8964861
Abstract

Efe Pygmies of northeast Zaire have the shortest mean adult stature of any population on earth. Although various alterations in the GH/insulin-like growth factor I (IGF-I) axis have been suggested, the basis for short stature in the Pygmy is unknown. We previously described IGF-I unresponsiveness in a T lymphoblast cell line derived from an Efe Pygmy, and studies in five additional lines have confirmed severe IGF-I resistance in these cells. We have now performed experiments to determine the molecular basis for the IGF-I resistance in these cells. We found markedly decreased cell surface expression of IGF-I receptors with normal ligand binding affinity. The Pygmy IGF-I receptors were not autophosphorylated and did not transmit a signal in response to physiological concentrations of IGF-I. There was a substantially decreased level of IGF-I receptor messenger ribonucleic acid in the Pygmy cells with a normal messenger ribonucleic acid half-life. The nucleotide sequence of the full-length IGF receptor complementary DNA in Pygmy 1 showed no significant variation. These results indicate decreased IGF-I receptor gene transcription and IGF-I receptor signaling as the primary variation in the Pygmy cell lines. The findings point to the IGF-I receptor as the locus governing short stature in the African Pygmy and suggest that human stature may be genetically controlled by expression of the IGF-I receptor.

摘要

扎伊尔东北部的埃菲俾格米人成年后的平均身高是地球上所有人种中最矮的。尽管有人提出生长激素/胰岛素样生长因子I(IGF-I)轴存在各种改变,但俾格米人身材矮小的原因尚不清楚。我们之前描述过从一名埃菲俾格米人身上获取的T淋巴母细胞系对IGF-I无反应,对另外五个细胞系的研究也证实了这些细胞对IGF-I具有严重抗性。我们现在进行了实验,以确定这些细胞中IGF-I抗性的分子基础。我们发现IGF-I受体的细胞表面表达显著降低,但其配体结合亲和力正常。俾格米人的IGF-I受体不会自动磷酸化,并且在生理浓度的IGF-I作用下不会传递信号。俾格米人细胞中IGF-I受体信使核糖核酸水平大幅降低,但其信使核糖核酸半衰期正常。俾格米人1号中全长IGF受体互补DNA的核苷酸序列没有明显变异。这些结果表明,IGF-I受体基因转录和IGF-I受体信号传导减少是俾格米人细胞系中的主要变异。这些发现表明IGF-I受体是控制非洲俾格米人身材矮小的基因位点,并提示人类身高可能由IGF-I受体的表达进行遗传控制。

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