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果蝇胰岛素受体含有一个新的羧基末端延伸,可能在信号转导中起重要作用。

The Drosophila insulin receptor contains a novel carboxyl-terminal extension likely to play an important role in signal transduction.

作者信息

Ruan Y, Chen C, Cao Y, Garofalo R S

机构信息

Department of Anatomy and Cell Biology, State University of New York, Health Science Center at Brooklyn 11203.

出版信息

J Biol Chem. 1995 Mar 3;270(9):4236-43. doi: 10.1074/jbc.270.9.4236.

Abstract

The nucleic acid and deduced amino acid sequence of the Drosophila insulin receptor homologue (dir) has been determined. The coding sequence of dir is contained within 10 exons spanning less than 8 kilobase pairs of genomic DNA. The deduced amino acid sequence of the dir encodes a protein of 2148 amino acids, larger than the human insulin receptor due to amino- and carboxyl-terminal extensions. The overall level of amino acid identity between the DIR and human insulin and insulin-like growth factor-I receptors is 32.5 and 33.3%, respectively. Higher levels of identity are found in exon 2 (45 and 43%, respectively) and in the beta subunit (50 and 48%, respectively), and the positions of most cysteine residues in the alpha subunit cysteine-rich domain are conserved. A novel, 400-amino acid, carboxyl-terminal extension contains 9 tyrosine residues, four of which are present in YXXM or YXXL motifs, suggesting that they function as binding sites for SH2 domain-containing signaling proteins. The presence of multiple putative SH2 domain binding sites in the DIR represents a significant difference from its mammalian homologues and suggests that, unlike the human insulin and insulin-like growth factor-I receptors, the DIR forms stable complexes with signaling molecules as part of its signal transduction mechanism.

摘要

果蝇胰岛素受体同源物(dir)的核酸及推导的氨基酸序列已被确定。dir的编码序列包含在10个外显子中,跨越的基因组DNA长度不到8千碱基对。推导的dir氨基酸序列编码一个2148个氨基酸的蛋白质,由于氨基端和羧基端的延伸,该蛋白质比人胰岛素受体更大。DIR与人胰岛素受体及胰岛素样生长因子-I受体之间的氨基酸整体一致性水平分别为32.5%和33.3%。在外显子2中(分别为45%和43%)以及β亚基中(分别为50%和48%)发现了更高的一致性水平,并且α亚基富含半胱氨酸结构域中大多数半胱氨酸残基的位置是保守的。一个新的、400个氨基酸的羧基端延伸含有9个酪氨酸残基,其中4个存在于YXXM或YXXL基序中,这表明它们作为含SH2结构域的信号蛋白的结合位点发挥作用。DIR中存在多个假定的SH2结构域结合位点,这与它的哺乳动物同源物存在显著差异,表明与人类胰岛素受体及胰岛素样生长因子-I受体不同,DIR作为其信号转导机制的一部分,能与信号分子形成稳定复合物。

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