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朊病毒蛋白的八肽重复区在 PrP(Sc)中构象发生改变。

The octarepeat region of the prion protein is conformationally altered in PrP(Sc).

机构信息

Research & Development, Novartis Vaccines & Diagnostics, Inc., Emeryville, California, United States of America.

出版信息

PLoS One. 2010 Feb 24;5(2):e9316. doi: 10.1371/journal.pone.0009316.

Abstract

BACKGROUND

Prion diseases are fatal neurodegenerative disorders characterized by misfolding and aggregation of the normal prion protein PrP(C). Little is known about the details of the structural rearrangement of physiological PrP(C) into a still-elusive disease-associated conformation termed PrP(Sc). Increasing evidence suggests that the amino-terminal octapeptide sequences of PrP (huPrP, residues 59-89), though not essential, play a role in modulating prion replication and disease presentation.

METHODOLOGY/PRINCIPAL FINDINGS: Here, we report that trypsin digestion of PrP(Sc) from variant and sporadic human CJD results in a disease-specific trypsin-resistant PrP(Sc) fragment including amino acids approximately 49-231, thus preserving important epitopes such as the octapeptide domain for biochemical examination. Our immunodetection analyses reveal that several epitopes buried in this region of PrP(Sc) are exposed in PrP(C).

CONCLUSIONS/SIGNIFICANCE: We conclude that the octapeptide region undergoes a previously unrecognized conformational transition in the formation of PrP(Sc). This phenomenon may be relevant to the mechanism by which the amino terminus of PrP(C) participates in PrP(Sc) conversion, and may also be exploited for diagnostic purposes.

摘要

背景

朊病毒病是致命的神经退行性疾病,其特征是正常朊病毒蛋白 PrP(C) 的错误折叠和聚集。关于生理 PrP(C) 结构重排为仍难以捉摸的疾病相关构象(称为 PrP(Sc))的详细信息知之甚少。越来越多的证据表明,尽管不是必需的,但 PrP 的氨基末端八肽序列(huPrP,残基 59-89)在调节朊病毒复制和疾病表现方面发挥作用。

方法/主要发现:在这里,我们报告说,来自变异型和散发性人类 CJD 的 PrP(Sc)的胰蛋白酶消化导致一种疾病特异性的胰蛋白酶抗性 PrP(Sc)片段,包括大约 49-231 个氨基酸,从而保留了用于生化检查的重要表位,如八肽结构域。我们的免疫检测分析表明,PrP(Sc) 中该区域埋藏的几个表位在 PrP(C) 中暴露。

结论/意义:我们得出结论,八肽区域在 PrP(Sc) 的形成过程中经历了以前未被识别的构象转变。这种现象可能与 PrP(C)的氨基末端参与 PrP(Sc)转化的机制有关,也可能被用于诊断目的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fed2/2827544/de21ba055a50/pone.0009316.g001.jpg

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