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宿主朊蛋白糖基化:决定朊病毒感染结果的主要因素。

Host PrP glycosylation: a major factor determining the outcome of prion infection.

作者信息

Tuzi Nadia L, Cancellotti Enrico, Baybutt Herbert, Blackford Lorraine, Bradford Barry, Plinston Chris, Coghill Anne, Hart Patricia, Piccardo Pedro, Barron Rona M, Manson Jean C

机构信息

Neuropathogenesis Unit, Roslin Institute, Edinburgh, United Kingdom.

出版信息

PLoS Biol. 2008 Apr 15;6(4):e100. doi: 10.1371/journal.pbio.0060100.

Abstract

The expression of the prion protein (PrP) is essential for transmissible spongiform encephalopathy (TSE) or prion diseases to occur, but the underlying mechanism of infection remains unresolved. To address the hypothesis that glycosylation of host PrP is a major factor influencing TSE infection, we have inoculated gene-targeted transgenic mice that have restricted N-linked glycosylation of PrP with three TSE strains. We have uniquely demonstrated that mice expressing only unglycosylated PrP can sustain a TSE infection, despite altered cellular location of the host PrP. Moreover we have shown that brain material from mice infected with TSE that have only unglycosylated PrP(Sc) is capable of transmitting infection to wild-type mice, demonstrating that glycosylation of PrP is not essential for establishing infection within a host or for transmitting TSE infectivity to a new host. We have further dissected the requirement of each glycosylation site and have shown that different TSE strains have dramatically different requirements for each of the glycosylation sites of host PrP, and moreover, we have shown that the host PrP has a major role in determining the glycosylation state of de novo generated PrP(Sc).

摘要

朊病毒蛋白(PrP)的表达是传染性海绵状脑病(TSE)或朊病毒疾病发生的必要条件,但感染的潜在机制仍未得到解决。为了验证宿主PrP糖基化是影响TSE感染的主要因素这一假说,我们用三种TSE毒株接种了PrP的N-连接糖基化受限的基因靶向转基因小鼠。我们独特地证明,尽管宿主PrP的细胞定位发生了改变,但仅表达未糖基化PrP的小鼠仍能维持TSE感染。此外,我们还表明,感染了仅具有未糖基化PrP(Sc)的TSE的小鼠的脑材料能够将感染传播给野生型小鼠,这表明PrP糖基化对于在宿主体内建立感染或向新宿主传播TSE传染性并非必不可少。我们进一步剖析了每个糖基化位点的需求,并表明不同的TSE毒株对宿主PrP的每个糖基化位点有截然不同的需求,此外,我们还表明宿主PrP在决定新生PrP(Sc)的糖基化状态方面起主要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/64da/2689698/8abc3c089ac9/pbio.0060100.g001.jpg

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