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不同 CWD 朊病毒株在基因靶向小鼠外周和脑内挑战过程中的传播。

Propagation of distinct CWD prion strains during peripheral and intracerebral challenges of gene-targeted mice.

机构信息

Prion Research Center, Department of Microbiology, Immunology, and Pathology, Colorado State University, Fort Collins, CO.

出版信息

Proc Natl Acad Sci U S A. 2024 Aug 6;121(32):e2402726121. doi: 10.1073/pnas.2402726121. Epub 2024 Jul 31.

Abstract

Since prion diseases result from infection and neurodegeneration of the central nervous system (CNS), experimental characterizations of prion strain properties customarily rely on the outcomes of intracerebral challenges. However, natural transmission of certain prions, including those causing chronic wasting disease (CWD) in elk and deer, depends on propagation in peripheral host compartments prior to CNS infection. Using gene-targeted GtE and GtQ mice, which accurately control cellular elk or deer PrP expression, we assessed the impact that peripheral or intracerebral exposures play on CWD prion strain propagation and resulting CNS abnormalities. Whereas oral and intraperitoneal transmissions produced identical neuropathological outcomes in GtE and GtQ mice and preserved the naturally convergent conformations of elk and deer CWD prions, intracerebral transmissions generated CNS prion strains with divergent biochemical properties in GtE and GtQ mice that were changed compared to their native counterparts. While CWD replication kinetics remained constant during iterative peripheral transmissions and brain titers reflected those found in native hosts, serial intracerebral transmissions produced 10-fold higher prion titers and accelerated incubation times. Our demonstration that peripherally and intracerebrally challenged Gt mice develop dissimilar CNS diseases which result from the propagation of distinct CWD prion strains points to the involvement of tissue-specific cofactors during strain selection in different host compartments. Since peripheral transmissions preserved the natural features of elk and deer prions, whereas intracerebral propagation produced divergent strains, our findings illustrate the importance of experimental characterizations using hosts that not only abrogate species barriers but also accurately recapitulate natural transmission routes of native strains.

摘要

由于朊病毒疾病是由中枢神经系统(CNS)的感染和神经退行性变引起的,因此对朊病毒株特性的实验表征通常依赖于脑内挑战的结果。然而,某些朊病毒的自然传播,包括引起麋鹿和鹿慢性消耗病(CWD)的朊病毒,取决于在 CNS 感染之前在周围宿主隔室中的传播。使用基因靶向的 GtE 和 GtQ 小鼠,这些小鼠可以准确控制细胞内麋鹿或鹿 PrP 的表达,我们评估了外周或脑内暴露对 CWD 朊病毒株传播和由此产生的 CNS 异常的影响。虽然口服和腹腔内传播在 GtE 和 GtQ 小鼠中产生了相同的神经病理学结果,并保留了麋鹿和鹿 CWD 朊病毒的自然趋同构象,但脑内传播在 GtE 和 GtQ 小鼠中产生了具有不同生化特性的 CNS 朊病毒株,与它们的天然对应物相比发生了变化。虽然 CWD 复制动力学在迭代的外周传播过程中保持不变,并且脑内滴度反映了在天然宿主中发现的那些,但连续的脑内传播导致 GtE 和 GtQ 小鼠中的朊病毒滴度增加了 10 倍,潜伏期缩短。我们的研究结果表明,外周和脑内 challenged Gt 小鼠会发展出不同的 CNS 疾病,这些疾病是由不同的 CWD 朊病毒株的传播引起的,这表明在不同的宿主隔室中,组织特异性辅助因子参与了株的选择。由于外周传播保留了麋鹿和鹿朊病毒的天然特征,而脑内传播产生了不同的株,我们的研究结果说明了使用不仅消除种间屏障而且还准确再现天然传播途径的宿主进行实验表征的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6d31/11317562/636719cd77df/pnas.2402726121fig01.jpg

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