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胰岛素样生长因子在胚胎及出生后生长中的作用。

Role of insulin-like growth factors in embryonic and postnatal growth.

作者信息

Baker J, Liu J P, Robertson E J, Efstratiadis A

机构信息

Department of Genetics and Development, Columbia University, New York, New York 10032.

出版信息

Cell. 1993 Oct 8;75(1):73-82.

PMID:8402902
Abstract

A developmental analysis of growth kinetics in mouse embryos carrying null mutations of the genes encoding insulin-like growth factor I (IGF-I), IGF-II, and the type 1 IGF receptor (IGF1R), alone or in combination, defined the onset of mutational effects leading to growth deficiency and indicated that between embryonic days 11.0 and 12.5, IGF1R serves only the in vivo mitogenic signaling of IGF-II. From E13.5 onward, IGF1R interacts with both IGF-I and IGF-II, while IGF-II recognizes an additional unknown receptor (XR). In contrast with the embryo proper, placental growth is served exclusively by an IGF-II-XR interaction. Additional genetic data suggested that the type 2IGF/mannose 6-phosphate receptor is an unlikely candidate for XR. Postnatal growth curves indicated that surviving Igf-1(-/-) mutants, which are infertile and exhibit delayed bone development, continue to grow with a retarded rate after birth in comparison with wild-type littermates and become 30% of normal weight as adults.

摘要

对携带胰岛素样生长因子I(IGF-I)、IGF-II和1型IGF受体(IGF1R)基因无效突变的小鼠胚胎单独或联合进行生长动力学的发育分析,确定了导致生长缺陷的突变效应的起始时间,并表明在胚胎第11.0天至12.5天之间,IGF1R仅介导IGF-II的体内促有丝分裂信号传导。从胚胎第13.5天起,IGF1R与IGF-I和IGF-II都相互作用,而IGF-II识别另一种未知受体(XR)。与胚胎本身不同,胎盘生长完全由IGF-II-XR相互作用介导。其他遗传数据表明,2型IGF/甘露糖6-磷酸受体不太可能是XR的候选者。出生后的生长曲线表明,存活下来的Igf-1(-/-)突变体不育且骨骼发育延迟,与野生型同窝仔相比,出生后生长速度仍然迟缓,成年后体重仅为正常体重的30%。

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