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表达多种 VSG 的非洲锥虫会被宿主免疫系统迅速清除。

African trypanosomes expressing multiple VSGs are rapidly eliminated by the host immune system.

机构信息

Instituto de Medicina Molecular-João Lobo Antunes, Faculdade de Medicina, Universidade de Lisboa, 1649-028 Lisboa, Portugal.

Division of Immune Diversity, German Cancer Research Center, 69120 Heidelberg, Germany.

出版信息

Proc Natl Acad Sci U S A. 2019 Oct 8;116(41):20725-20735. doi: 10.1073/pnas.1905120116. Epub 2019 Sep 25.

Abstract

parasites successfully evade the host immune system by periodically switching the dense coat of variant surface glycoprotein (VSG) at the cell surface. Each parasite expresses in a monoallelic fashion that is tightly regulated. The consequences of exposing multiple VSGs during an infection, in terms of antibody response and disease severity, remain unknown. In this study, we overexpressed a high-mobility group box protein, TDP1, which was sufficient to open the chromatin of silent expression sites, to disrupt monoallelic expression, and to generate viable and healthy parasites with a mixed VSG coat. Mice infected with these parasites mounted a multi-VSG antibody response, which rapidly reduced parasitemia. Consequently, we observed prolonged survival in which nearly 90% of the mice survived a 30-d period of infection with undetectable parasitemia. Immunodeficient RAG2 knock-out mice were unable to control infection with TDP1-overexpressing parasites, showing that the adaptive immune response is critical to reducing disease severity. This study shows that simultaneous exposure of multiple VSGs is highly detrimental to the parasite, even at the very early stages of infection, suggesting that drugs that disrupt VSG monoallelic expression could be used to treat trypanosomiasis.

摘要

寄生虫通过周期性地改变细胞表面密集的变异表面糖蛋白 (VSG) 来成功逃避宿主免疫系统。每个寄生虫以单等位基因的方式表达,这种表达受到严格调控。在感染过程中暴露多种 VSG 会对抗体反应和疾病严重程度产生什么影响,目前尚不清楚。在这项研究中,我们过表达了一种高迁移率族蛋白框蛋白 TDP1,它足以打开沉默 表达位点的染色质,破坏 单等位基因表达,并产生具有混合 VSG 外壳的可行且健康的寄生虫。感染这些寄生虫的小鼠产生了多 VSG 抗体反应,这迅速降低了寄生虫血症。因此,我们观察到了更长的存活时间,近 90%的小鼠在感染期间未检测到寄生虫血症,存活了 30 天。免疫缺陷型 RAG2 敲除小鼠无法控制 TDP1 过表达寄生虫的感染,表明适应性免疫反应对于降低疾病严重程度至关重要。这项研究表明,即使在感染的早期阶段,同时暴露多种 VSG 对寄生虫也是非常有害的,这表明破坏 VSG 单等位基因表达的药物可用于治疗锥虫病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e868/6789922/5d496d76ded4/pnas.1905120116fig01.jpg

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