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淋巴滤泡微环境是朊病毒病绵羊慢性炎症组织中病理性朊病毒蛋白沉积所必需的。

A lympho-follicular microenvironment is required for pathological prion protein deposition in chronically inflamed tissues from scrapie-affected sheep.

机构信息

Dipartimento di Sanità Animale, Istituto Zooprofilattico Sperimentale della Sardegna, Sassari, Italy.

出版信息

PLoS One. 2013 May 3;8(5):e62830. doi: 10.1371/journal.pone.0062830. Print 2013.

Abstract

In sheep scrapie, pathological prion protein (PrP(Sc)) deposition occurs in the lymphoreticular and central nervous systems. We investigated PrP(Sc) distribution in scrapie-affected sheep showing simultaneous evidence of chronic lymphofollicular, lymphoproliferative/non-lymphofollicular, and/or granulomatous inflammations in their mammary gland, lung, and ileum. To do this, PrP(Sc) detection was carried out via immunohistochemistry and Western Blotting techniques, as well as through inflammatory cell immunophenotyping. Expression studies of gene coding for biological factors modulating the host's inflammatory response were also carried out. We demonstrated that ectopic PrP(Sc) deposition occurs exclusively in the context of lymphofollicular inflammatory sites, inside newly formed and well-organized lymphoid follicles harboring follicular dendritic cells. On the contrary, no PrP(Sc) deposition was detected in granulomas, even when they were closely located to newly formed lymphoid follicles. A significantly more consistent expression of lymphotoxin α and β mRNA was detected in lymphofollicular inflammation compared to the other two types, with lymphotoxin α and β signaling new lymphoid follicles' formation and, likely, the occurrence of ectopic PrP(Sc) deposition inside them. Our findings suggest that, in sheep co-affected by scrapie and chronic inflammatory conditions, only newly formed lymphoid follicles provide a suitable micro-environment that supports the scrapie agent's replication in inflammatory sites, with an increased risk of prion shedding through body secretions/excretions.

摘要

在绵羊瘙痒病中,病理性朊病毒蛋白(PrP(Sc))沉积发生在淋巴网状和中枢神经系统中。我们研究了在其乳腺、肺和回肠中同时存在慢性淋巴滤泡、淋巴增生/非淋巴滤泡和/或肉芽肿炎症证据的瘙痒病感染绵羊中 PrP(Sc)的分布。为此,我们通过免疫组织化学和 Western Blotting 技术以及炎症细胞免疫表型分析来检测 PrP(Sc)。我们还进行了编码调节宿主炎症反应的生物学因子的基因表达研究。我们证明,异位 PrP(Sc)沉积仅发生在淋巴滤泡炎症部位,在新形成的、组织良好的含有滤泡树突状细胞的淋巴滤泡内。相反,在肉芽肿中未检测到 PrP(Sc)沉积,即使它们与新形成的淋巴滤泡紧密相邻。与其他两种类型相比,在淋巴滤泡炎症中检测到淋巴毒素 α 和 β mRNA 的表达更为一致,淋巴毒素 α 和 β 信号新的淋巴滤泡形成,并且可能在其中发生异位 PrP(Sc)沉积。我们的研究结果表明,在同时感染瘙痒病和慢性炎症的绵羊中,只有新形成的淋巴滤泡提供了一个合适的微环境,支持在炎症部位复制瘙痒病病原体,通过身体分泌物/排泄物释放朊病毒的风险增加。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1405/3643908/06b07f4d0b8c/pone.0062830.g001.jpg

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