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经皮肤暴露后的羊瘙痒症传播依赖于淋巴组织中的滤泡树突状细胞。

Scrapie transmission following exposure through the skin is dependent on follicular dendritic cells in lymphoid tissues.

作者信息

Mohan Joanne, Brown Karen L, Farquhar Christine F, Bruce Moira E, Mabbott Neil A

机构信息

Institute for Animal Health, Ogston Building, West Mains Road, Edinburgh EH9 3JF, UK.

出版信息

J Dermatol Sci. 2004 Aug;35(2):101-11. doi: 10.1016/j.jdermsci.2004.05.005.

Abstract

BACKGROUND

Transmissible spongiform encephalopathies (TSEs) are chronic infectious neurodegenerative diseases that are characterized by the accumulation in affected tissues of PrP(Sc), an abnormal isoform of the host prion protein (PrP(c)). Following peripheral exposure, PrP(Sc) usually accumulates on follicular dendritic cells (FDCS) in lymphoid tissues before neuroinvasion. Studies in mice have shown that TSE exposure through scarified skin is an effective means of transmission. Following inoculation via the skin, a functional immune system is critical for the transmission of scrapie to the brain as severe combined immunodeficiency (SCID) mice are refractory to infection. Until now, it was not known which components of the immune system are required for efficient scrapie neuroinvasion following skin scarification.

OBJECTIVE

To determine which cells are critical for the transmission of scrapie to the brain following inoculation via the skin.

METHODS

A chimeric mouse model was used, which had a mismatch in PrP(c) expression between FDCs and other bone marrow-derived cells within lymphoid tissues. These chimeric mice were challenged with scrapie by skin scarification to allow the separate roles of FDCs and lymphocytes in peripheral scrapie pathogenesis to be determined.

RESULTS

We show that mature FDCs are essential for the accumulation of scrapie within lymphoid tissues and the subsequent transmission of infection to the brain following TSE exposure by this route. Furthermore, we show that the accumulation of PrP(Sc) and infectivity in the spleen is independent of PrP expression by lymphocytes or other bone marrow-derived cells.

CONCLUSION

Following inoculation with scrapie by skin scarification, replication in the spleen and subsequent neuroinvasion is critically dependent upon mature FDCs.

摘要

背景

传染性海绵状脑病(TSEs)是慢性传染性神经退行性疾病,其特征是在受影响组织中积累PrP(Sc),即宿主朊病毒蛋白(PrP(c))的异常异构体。外周暴露后,PrP(Sc)通常在神经侵袭之前在淋巴组织的滤泡树突状细胞(FDCs)上积累。小鼠研究表明,通过划破皮肤暴露于TSE是一种有效的传播方式。经皮肤接种后,功能性免疫系统对于将羊瘙痒病传播到大脑至关重要,因为严重联合免疫缺陷(SCID)小鼠对感染具有抗性。到目前为止,尚不清楚在划破皮肤后高效的羊瘙痒病神经侵袭需要免疫系统的哪些成分。

目的

确定经皮肤接种后哪些细胞对于将羊瘙痒病传播到大脑至关重要。

方法

使用一种嵌合小鼠模型,其淋巴组织内FDCs与其他骨髓来源细胞之间的PrP(c)表达不匹配。通过划破皮肤用羊瘙痒病攻击这些嵌合小鼠,以确定FDCs和淋巴细胞在周围性羊瘙痒病发病机制中的各自作用。

结果

我们表明,成熟的FDCs对于羊瘙痒病在淋巴组织内的积累以及通过该途径暴露于TSE后随后将感染传播到大脑至关重要。此外,我们表明脾脏中PrP(Sc)和传染性的积累与淋巴细胞或其他骨髓来源细胞的PrP表达无关。

结论

经皮肤划破接种羊瘙痒病后,在脾脏中的复制以及随后的神经侵袭严重依赖于成熟的FDCs。

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