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牛痘病毒蛋白 N1 抑制固有免疫可促进皮肤微生物组扩张,并增加疫苗接种后的免疫浸润。

Suppression of innate immunity by the vaccinia virus protein N1 promotes skin microbiota expansion and increased immune infiltration following vaccination.

机构信息

Department of Pathology, University of Cambridge, Cambridge, UK.

Present address: Department of Biology, Tufts University, Medford, Massachusetts, USA.

出版信息

J Gen Virol. 2022 Nov;103(11). doi: 10.1099/jgv.0.001814.

Abstract

Vaccinia virus (VACV) protein N1 is an intracellular immunomodulator that contributes to virus virulence via inhibition of NF-κB. Intradermal infection with a VACV lacking gene (vΔN1) results in smaller skin lesions than infection with wild-type virus (WT VACV), but the impact of N1 deletion on the local microbiota as well as the innate and cellular immune responses in infected ear tissue is mostly uncharacterized. Here, we analysed the bacterial burden and host immune response at the site of infection and report that the presence of protein N1 correlated with enhanced expansion of skin microbiota, even before lesion development. Furthermore, early after infection (days 1-3), prior to lesion development, the levels of inflammatory mediators were higher in vΔN1-infected tissue compared to WT VACV infection. In contrast, infiltration of ear tissue with myeloid and lymphoid cells was greater after WT VACV infection and there was significantly greater secondary bacterial infection that correlated with greater lesion size. We conclude that a more robust innate immune response to vΔN1 infection leads to better control of virus replication, less bacterial growth and hence an overall reduction of tissue damage and lesion size. This analysis shows the potent impact of a single viral immunomodulator on the host immune response and the pathophysiology of VACV infection in the skin.

摘要

牛痘病毒(VACV)蛋白 N1 是一种细胞内免疫调节剂,通过抑制 NF-κB 促进病毒毒力。与野生型病毒(WT VACV)相比,经皮感染缺乏基因(vΔN1)的 VACV 会导致皮肤损伤更小,但 N1 缺失对感染耳组织中局部微生物群以及固有和细胞免疫反应的影响在很大程度上仍未得到描述。在这里,我们分析了感染部位的细菌负担和宿主免疫反应,并报告说 N1 蛋白的存在与皮肤微生物群的扩张增强相关,甚至在病变发展之前。此外,在感染早期(第 1-3 天),在病变发展之前,vΔN1 感染组织中的炎症介质水平高于 WT VACV 感染。相比之下,WT VACV 感染后,耳组织中髓样和淋巴样细胞的浸润更多,并且存在更大的继发性细菌感染,这与更大的病变大小相关。我们得出结论,对 vΔN1 感染的更强烈的固有免疫反应导致更好地控制病毒复制、更少的细菌生长,从而整体减少组织损伤和病变大小。这项分析表明,单一病毒免疫调节剂对宿主免疫反应和 VACV 在皮肤中的病理生理学有很大影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e614/7614846/ddedb55143f9/EMS179319-f001.jpg

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