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曼氏血吸虫一种不同寻常的受体酪氨酸激酶含有一个捕蝇草模块。

An unusual receptor tyrosine kinase of Schistosoma mansoni contains a Venus Flytrap module.

作者信息

Vicogne Jérôme, Pin Jean Philippe, Lardans Vinca, Capron Monique, Noël Christophe, Dissous Colette

机构信息

Unité INSERM 547, Institut Pasteur Lille, 1 rue du Pr. Calmette, France.

出版信息

Mol Biochem Parasitol. 2003 Jan;126(1):51-62. doi: 10.1016/s0166-6851(02)00249-9.

Abstract

Previous studies have suggested that successful development of the parasitic helminth Schistosoma mansoni must be dependent on an adaptative molecular dialogue with its hosts and on the existence of receptors for growth factors and hormones. Attempts to identify a homolog of the insulin receptor (IR) have led us to characterize a new receptor tyrosine kinase (RTK) molecule in S. mansoni. SmRTK-1 is an integral membrane protein with a single membrane-spanning sequence separating an extracellular ligand-binding domain and a cytoplasmic TK domain. Structural and phylogenetic analyses of the kinase domain of SmRTK-1 confirmed its similarity to IR catalytic domains. However, sequence analysis of the extracellular domain of SmRTK-1 revealed similarity with various proteins (such as drug receptors) that share a structure known as the Venus Flytrap (VFT) module. Alignment with other VFT modules for which the structure has been solved was used to generate a 3D model of the putative VFT module of SmRTK-1. Phylogenetic analysis indicated that the SmRTK-1 VFT module was closer to that of the GABA(B) receptor. Numerous RTK genes recently discovered in vertebrate and invertebrate species code for large families of modular proteins with diverse structures and ligand-binding specificities. SmRTK-1 probably represents a new class of RTK whose function remains to be determined. RTKs are present in all metazoans and associated with the control of metabolism, growth and development. The preferential localization of SmRTK-1 in sporocyst germinal cells and ovocytes could be in favor of its function in schistosome growth and differentiation.

摘要

先前的研究表明,曼氏血吸虫这种寄生性蠕虫的成功发育必定依赖于与宿主的适应性分子对话以及生长因子和激素受体的存在。对胰岛素受体(IR)同源物的鉴定尝试使我们在曼氏血吸虫中鉴定出一种新的受体酪氨酸激酶(RTK)分子。SmRTK-1是一种整合膜蛋白,具有单个跨膜序列,该序列将细胞外配体结合域和细胞质TK域分隔开。对SmRTK-1激酶结构域的结构和系统发育分析证实了它与IR催化结构域的相似性。然而,对SmRTK-1细胞外结构域的序列分析揭示了它与各种具有一种称为捕蝇草(VFT)模块结构的蛋白质(如药物受体)的相似性。将其与已解析结构的其他VFT模块进行比对,以生成SmRTK-1假定VFT模块的三维模型。系统发育分析表明,SmRTK-1的VFT模块与GABA(B)受体的VFT模块更为接近。最近在脊椎动物和无脊椎动物物种中发现的众多RTK基因编码具有不同结构和配体结合特异性的模块化蛋白大家族。SmRTK-1可能代表了一类功能尚待确定的新型RTK。RTK存在于所有后生动物中,并与新陈代谢、生长和发育的控制相关。SmRTK-1在胞蚴生殖细胞和卵母细胞中的优先定位可能有利于其在血吸虫生长和分化中的功能。

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