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朊蛋白N端结构域触发Dpl的朊蛋白(Sc)样聚集。

PrP N-terminal domain triggers PrP(Sc)-like aggregation of Dpl.

作者信息

Erlich Paul, Cesbron Jean-Yves, Lemaire-Vieille Catherine, Curt Aurélie, Andrieu Jean-Pierre, Schoehn Guy, Jamin Marc, Gagnon Jean

机构信息

Laboratoire Adaptation et Pathogénie des Micro-organismes, Université Joseph Fourier, BP 170, 38042 Grenoble Cedex 9, France.

出版信息

Biochem Biophys Res Commun. 2008 Jan 18;365(3):478-83. doi: 10.1016/j.bbrc.2007.10.202. Epub 2007 Nov 13.

Abstract

Transmissible spongiform encephalopathies are fatal neurodegenerative disorders thought to be transmitted by self-perpetuating conformational conversion of a neuronal membrane glycoprotein (PrP(C), for "cellular prion protein") into an abnormal state (PrP(Sc), for "scrapie prion protein"). Doppel (Dpl) is a protein that shares significant biochemical and structural homology with PrP(C). In contrast to its homologue PrP(C), Dpl is unable to participate in prion disease progression or to achieve an abnormal PrP(Sc)-like state. We have constructed a chimeric mouse protein, composed of the N-terminal domain of PrP(C) (residues 23-125) and the C-terminal part of Dpl (residues 58-157). This chimeric protein displays PrP-like biochemical and structural features; when incubated in presence of NaCl, the alpha-helical monomer forms soluble beta-sheet-rich oligomers which acquire partial resistance to pepsin proteolysis in vitro, as do PrP oligomers. Moreover, the presence of aggregates akin to protofibrils is observed in soluble oligomeric species by electron microscopy.

摘要

传染性海绵状脑病是致命的神经退行性疾病,被认为是由神经元膜糖蛋白(PrP(C),即“细胞朊蛋白”)自我持续的构象转变为异常状态(PrP(Sc),即“瘙痒病朊蛋白”)而传播的。多普蛋白(Dpl)是一种与PrP(C)具有显著生化和结构同源性的蛋白质。与其同源物PrP(C)不同,Dpl无法参与朊病毒疾病的进展,也无法达到类似异常PrP(Sc)的状态。我们构建了一种嵌合小鼠蛋白,它由PrP(C)的N端结构域(第23 - 125位氨基酸残基)和Dpl的C端部分(第58 - 157位氨基酸残基)组成。这种嵌合蛋白具有类似PrP的生化和结构特征;当在氯化钠存在的情况下孵育时,α - 螺旋单体形成富含β - 折叠的可溶性寡聚体,在体外对胃蛋白酶消化具有部分抗性,PrP寡聚体也是如此。此外,通过电子显微镜观察到可溶性寡聚体中有类似于原纤维的聚集体存在。

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