首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Recognition of the tumor suppressor protein p53 and other protein targets by the calcium-binding protein S100B
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Recognition of the tumor suppressor protein p53 and other protein targets by the calcium-binding protein S100B

机译:钙结合蛋白S100B对肿瘤抑制蛋白p53和其他蛋白靶标的识别

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S100B is an EF-hand containing calcium-binding protein of the S100 protein family that exerts its biological effect by binding and affecting various target proteins. A consensus sequence for S100B target proteins was published as (K/R)(L/I)xWxxIL and matches a region in the actin capping protein CapZ (VV. Ivanenkov, G.A. Jamieson, Jr., E. Gruenstein, R.V. Dimlich, Characterization of S-100b binding epitopes. Identification of a novel target, the actin capping protein, CapZ, J. Biol. Chem. 270 (1995) 14651-14658). Several additional S100B targets are known including p53, a nuclear Dbf2 related (NDR) kinase, the RAGE receptor, neuromodulin, protein kinase C, and others. Examining the binding sites of such targets and new protein sequence searches provided additional potential target proteins for S100B including Hdm2 and Hdm4, which were both found to bind S100B in a calcium-dependent manner. The interaction between S100B and the Hdm2 and/or the Hdm4 proteins may be important physiologically in light of evidence that like Hdm2, S100B also contributes to lowering protein levels of the tumor suppressor protein, p53. For the S100B-p53 interaction, it was found that phosphorylation of specific serine and/or threonine residues reduces the affinity of the S10B-p53 interaction by as much as an order of magnitude, and is important for protecting p53 from S100B-dependent downregulation, a scenario that is similar to what is found for the Hdm2-p53 complex. (c) 2006 Elsevier B.V. All rights reserved.
机译:S100B是包含S100蛋白家族的钙结合蛋白的EF手,它通过结合并影响各种靶蛋白发挥其生物学作用。 S100B目标蛋白的共有序列以(K / R)(L / I)xWxxIL的形式发布,并与肌动蛋白加帽蛋白CapZ中的一个区域匹配(VV.Ivanenkov,GA Jamieson,Jr.,E.Gruenstein,RV Dimlich,表征S-100b结合表位的鉴定,新靶标,肌动蛋白封端蛋白的鉴定,CapZ,J.Biol.Chem.270(1995)14651-14658)。已知有几个其他的S100B靶标,包括p53,与Dbf2相关的核(NDR)激酶,RAGE受体,神经调节蛋白,蛋白激酶C等。检查此类靶标的结合位点并进行新的蛋白质序列搜索可提供S100B的其他潜在靶标蛋白,包括Hdm2和Hdm4,它们均以钙依赖性方式结合S100B。 S100B与Hdm2和/或Hdm4蛋白之间的相互作用在生理上可能很重要,因为有证据表明S100B像Hdm2一样也有助于降低肿瘤抑制蛋白p53的蛋白水平。对于S100B-p53相互作用,发现特定丝氨酸和/或苏氨酸残基的磷酸化将S10B-p53相互作用的亲和力降低了一个数量级,并且对于保护p53不受S100B依赖性下调很重要,一种类似于Hdm2-p53复合体的方案。 (c)2006 Elsevier B.V.保留所有权利。

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