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对黑腹果蝇糙面突变等位基因的分子分析表明,有一种具有两个功能域的分泌蛋白。

Molecular analysis of scabrous mutant alleles from Drosophila melanogaster indicates a secreted protein with two functional domains.

作者信息

Hu X, Lee E C, Baker N E

机构信息

Department of Molecular Genetics, Albert Einstein College of Medicine, Bronx, New York 10461, USA.

出版信息

Genetics. 1995 Oct;141(2):607-17. doi: 10.1093/genetics/141.2.607.

Abstract

Mutations at the scabrous locus (sca) affect cell-cell signaling during neural development. Twenty-one mutant alleles of scabrous have been analyzed. Many synthesize no sca protein. In others, a defective protein is arrested intracellularly. Two mutants in which protein is not arrested must affect sca protein function outside the cell. Both affect the fibrinogen related domain (FReD), a 200-amino acid segment conserved in fibrinogen, tenascins, and other proteins. In fibrinogen, this region is involved in protein interactions and is altered in human mutations affecting blood clotting. In sca(UM2), an invariant Asp residue is replaced by Asn. In sca(MSKF) allele has dominant negative properties, indicating that the truncated amino-terminal portion interferes with the function of so me other gene product. These mutations show that the conserved FReD is essential for wild-type sca function, but suggest that the amino-terminal domain also interacts with other proteins, but other neural mutations were without effect. Models for the role of a two-domain protein in neural development are discussed.

摘要

粗糙位点(sca)的突变会影响神经发育过程中的细胞间信号传导。现已分析了21个粗糙位点的突变等位基因。许多突变体不合成sca蛋白。在其他突变体中,有缺陷的蛋白在细胞内被滞留。有两个突变体,其蛋白没有被滞留,必定是影响了细胞外的sca蛋白功能。这两个突变体都影响纤维蛋白原相关结构域(FReD),这是在纤维蛋白原、腱生蛋白和其他蛋白中保守的一段200个氨基酸的序列。在纤维蛋白原中,该区域参与蛋白质相互作用,并且在影响血液凝固的人类突变中会发生改变。在sca(UM2)中,一个不变的天冬氨酸残基被天冬酰胺取代。sca(MSKF)等位基因具有显性负性特性,表明截短的氨基末端部分会干扰某些其他基因产物的功能。这些突变表明,保守的FReD对于野生型sca功能至关重要,但也表明氨基末端结构域也与其他蛋白质相互作用,不过其他神经突变没有产生影响。文中讨论了一种双结构域蛋白在神经发育中的作用模型。

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