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HIV-1的补体调理作用通过CR3导致未成熟树突状细胞的抗病毒和炎症反应降低。

Complement opsonization of HIV-1 results in decreased antiviral and inflammatory responses in immature dendritic cells via CR3.

作者信息

Ellegård Rada, Crisci Elisa, Burgener Adam, Sjöwall Christopher, Birse Kenzie, Westmacott Garrett, Hinkula Jorma, Lifson Jeffrey D, Larsson Marie

机构信息

Division of Molecular Virology, Department of Clinical and Experimental Medicine, Linköping University, 581 85 Linköping, Sweden;

Department of Medical Microbiology, University of Manitoba, Winnipeg, Manitoba R3E 0J9, Canada; National Microbiology Laboratory, Public Health Agency of Canada, Winnipeg, Manitoba R3E 3R2, Canada;

出版信息

J Immunol. 2014 Nov 1;193(9):4590-601. doi: 10.4049/jimmunol.1401781. Epub 2014 Sep 24.

DOI:10.4049/jimmunol.1401781
PMID:25252956
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4201991/
Abstract

Immature dendritic cells (iDCs) in genital and rectal mucosa may be one of the first cells to come into contact with HIV-1 during sexual transmission of virus. HIV-1 activates the host complement system, which results in opsonization of virus by inactivated complement fragments, for example, iC3b. We investigated antiviral and inflammatory responses induced in human iDCs after exposure to free HIV-1 (F-HIV), complement-opsonized HIV-1 (C-HIV), and complement and Ab-opsonized HIV-1 (CI-HIV). F-HIV gave rise to a significantly higher expression of antiviral factors such as IFN-β, myxovirus resistance protein A, and IFN-stimulated genes, compared with C-HIV and CI-HIV. Additionally, F-HIV induced inflammatory factors such as IL-1β, IL-6, and TNF-α, whereas these responses were weakened or absent after C-HIV or CI-HIV exposure. The responses induced by F-HIV were TLR8-dependent with subsequent activation of IFN regulatory factor 1, p38, ERK, PI3K, and NF-κB pathways, whereas these responses were not induced by C-HIV, which instead induced activation of IFN regulatory factor 3 and Lyn. This modulation of TLR8 signaling was mediated by complement receptor 3 and led to enhanced infection. The impact that viral hijacking of the complement system has on iDC function could be an important immune evasion mechanism used by HIV-1 to establish infection in the host.

摘要

生殖器和直肠黏膜中的未成熟树突状细胞(iDCs)可能是病毒性传播过程中最早接触HIV-1的细胞之一。HIV-1激活宿主补体系统,导致病毒被灭活的补体片段(如iC3b)调理。我们研究了人iDCs在暴露于游离HIV-1(F-HIV)、补体调理的HIV-1(C-HIV)以及补体和抗体调理的HIV-1(CI-HIV)后诱导产生的抗病毒和炎症反应。与C-HIV和CI-HIV相比,F-HIV能显著上调抗病毒因子如IFN-β、抗黏液病毒蛋白A和IFN刺激基因的表达。此外,F-HIV诱导炎症因子如IL-1β、IL-6和TNF-α的产生,而C-HIV或CI-HIV暴露后这些反应减弱或缺失。F-HIV诱导的反应依赖于TLR8,随后激活IFN调节因子1、p38、ERK、PI3K和NF-κB通路,而C-HIV不诱导这些反应,而是诱导IFN调节因子3和Lyn的激活。TLR8信号的这种调节由补体受体3介导,并导致感染增强。病毒对补体系统的劫持对iDC功能的影响可能是HIV-1在宿主体内建立感染所采用的一种重要免疫逃避机制。