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首页> 外文期刊>Biochimica et Biophysica Acta. Protein Structure and Molecular Enzymology >Structure-function relationships in the ezrin family and the effect of tumor-associated point mutations in neurofibromatosis 2 protein
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Structure-function relationships in the ezrin family and the effect of tumor-associated point mutations in neurofibromatosis 2 protein

机译:ezrin家族中的结构功能关系和神经纤维瘤病2蛋白中肿瘤相关的点突变的影响

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摘要

Ezrin, radixin and moesin (ERM proteins) link cell adhesion molecules to the cytoskeleton, modulate cell morphology and cell growth and are involved in Rho-mediated signal transduction. Merlin, the tumor suppressor in neurofibromatosis 2, is a diverged member of the ezrin family, but its function is at least partially similar to the ERM proteins. In the N-domain, the ezrin family belongs to the band 4.1 superfamily. Secondary structure predictions made separately for the ezrin and band 4.1-tyrosine phosphatase families give a similar pattern for the homologous N-domains, indicating that both families have a similar binding site for the integral membrane proteins. The α-domain shows a strong coiled-coil prediction, that can be involved in the protein dimerization. The C-terminal actin-binding site in the ERM proteins and the actin-binding helix in the villin headpiece have a common amino acid motif. In merlin, the published tumor-associated single amino acid mutations in the N-domain are located in the conserved sites, and they affect mainly the predicted helices and strands, indicating that these mutations cause the disease primarily by disturbing the protein structure. In the α- and C-domains, some of the mutations break the helical structures. Some known mutations are observed at a site potentially interacting with cell adhesion molecules. We will also discuss the implications of the evolutionary information and the actin-binding models in the ezrin family.
机译:Ezrin,Radixin和Moesin(ERM蛋白)将细胞粘附分子连接至细胞骨架,调节细胞形态和细胞生长,并参与Rho介导的信号转导。 Merlin是神经纤维瘤病2中的肿瘤抑制因子,是ezrin家族的成员,但其功能至少部分类似于ERM蛋白。在N域中,ezrin家族属于4.1乐队。分别针对ezrin和4.1带酪氨酸磷酸酶家族进行的二级结构预测为同源N结构域提供了相似的模式,表明这两个家族对于整合膜蛋白具有相似的结合位点。 α结构域显示出强大的卷曲螺旋预测,这可能与蛋白质二聚化有关。 ERM蛋白中的C端肌动蛋白结合位点和villin头饰中的肌动蛋白结合螺旋具有共同的氨基酸基序。在merlin中,已发表的N结构域中与肿瘤相关的单个氨基酸突变位于保守位点,它们主要影响预测的螺旋和链,表明这些突变主要通过干扰蛋白质结构来引起疾病。在α和C结构域,某些突变破坏了螺旋结构。在可能与细胞粘附分子相互作用的位点观察到一些已知的突变。我们还将讨论ezrin家族中进化信息和肌动蛋白结合模型的意义。

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