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发育调控因子HMGI-C中导致小鼠侏儒表型的突变。

Mutation responsible for the mouse pygmy phenotype in the developmentally regulated factor HMGI-C.

作者信息

Zhou X, Benson K F, Ashar H R, Chada K

机构信息

Department of Biochemistry, UMDNJ-Robert Wood Johnson Medical School, Piscataway 08854-5635, USA.

出版信息

Nature. 1995 Aug 31;376(6543):771-4. doi: 10.1038/376771a0.

Abstract

Growth is one of the fundamental aspects in the development of an organism. Classical genetic studies have isolated four viable, spontaneous mouse mutants disrupted in growth, leading to dwarfism. Pygmy is unique among these mutants because its phenotype cannot be explained by aberrations in the growth hormone-insulin-like growth factor endocrine pathway. Here we show that the pygmy phenotype arises from the inactivation of Hmgi-c (ref. 6), a member of the Hmgi family which function as architectural factors in the nuclear scaffold and are critical in the assembly of stereospecific transcriptional complexes. Hmgi-c and another Hmgi family member, Hmgi(gamma) (ref. 10), were found to be expressed predominantly during embryogenesis. The HMGI proteins are known to be regulated by cell cycle-dependent phosphorylation which alters their DNA binding affinity. These results demonstrate the important role of HMGI proteins in mammalian growth and development.

摘要

生长是生物体发育的基本方面之一。经典遗传学研究已分离出四种在生长过程中发生破坏的、可存活的自发小鼠突变体,导致侏儒症。侏儒小鼠在这些突变体中是独特的,因为其表型无法通过生长激素 - 胰岛素样生长因子内分泌途径的畸变来解释。在这里,我们表明侏儒小鼠的表型源于Hmgi - c(参考文献6)的失活,Hmgi - c是Hmgi家族的成员,在核支架中作为结构因子起作用,并且在立体特异性转录复合物的组装中起关键作用。发现Hmgi - c和另一个Hmgi家族成员Hmgi(γ)(参考文献10)主要在胚胎发生过程中表达。已知HMGI蛋白受细胞周期依赖性磷酸化调节,这会改变它们与DNA的结合亲和力。这些结果证明了HMGI蛋白在哺乳动物生长和发育中的重要作用。

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