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猫白血病病毒感染人类细胞的障碍:对人畜共患病抗性的见解。

Barriers to Infection of Human Cells by Feline Leukemia Virus: Insights into Resistance to Zoonosis.

作者信息

Terry Anne, Kilbey Anna, Naseer Asif, Levy Laura S, Ahmad Shamim, Watts Ciorsdaidh, Mackay Nancy, Cameron Ewan, Wilson Sam, Neil James C

机构信息

MRC University of Glasgow Centre for Virus Research, University of Glasgow, Glasgow, United Kingdom.

Tulane University, New Orleans, Louisiana, USA.

出版信息

J Virol. 2017 Feb 14;91(5). doi: 10.1128/JVI.02119-16. Print 2017 Mar 1.

Abstract

The human genome displays a rich fossil record of past gammaretrovirus infections, yet no current epidemic is evident, despite environmental exposure to viruses that infect human cells Feline leukemia viruses (FeLVs) rank high on this list, but neither domestic nor workplace exposure has been associated with detectable serological responses. Nonspecific inactivation of gammaretroviruses by serum factors appears insufficient to explain these observations. To investigate further, we explored the susceptibilities of primary and established human cell lines to FeLV-B, the most likely zoonotic variant. Fully permissive infection was common in cancer-derived cell lines but was also a feature of nontransformed keratinocytes and lung fibroblasts. Cells of hematopoietic origin were generally less permissive and formed discrete groups on the basis of high or low intracellular protein expression and virion release. Potent repression was observed in primary human blood mononuclear cells and a subset of leukemia cell lines. However, the early steps of reverse transcription and integration appear to be unimpaired in nonpermissive cells. FeLV-B was subject to G→A hypermutation with a predominant APOBEC3G signature in partially permissive cells but was not mutated in permissive cells or in nonpermissive cells that block secondary viral spread. Distinct cellular barriers that protect primary human blood cells are likely to be important in protection against zoonotic infection with FeLV. Domestic exposure to gammaretroviruses such as feline leukemia viruses (FeLVs) occurs worldwide, but the basis of human resistance to infection remains incompletely understood. The potential threat is evident from the human genome sequence, which reveals many past epidemics of gammaretrovirus infection, and from recent cross-species jumps of gammaretroviruses from rodents to primates and marsupials. This study examined resistance to infection at the cellular level with the most prevalent human cell-tropic FeLV variant, FeLV-B. We found that blood cells are uniquely resistant to infection with FeLV-B due to the activity of cellular enzymes that mutate the viral genome. A second block, which appears to suppress viral gene expression after the viral genome has integrated into the host cell genome, was identified. Since cells derived from other normal human cell types are fully supportive of FeLV replication, innate resistance of blood cells could be critical in protecting against cross-species infection.

摘要

人类基因组显示出过去γ逆转录病毒感染的丰富化石记录,然而,尽管环境中存在感染人类细胞的病毒,但目前并没有明显的疫情爆发。猫白血病病毒(FeLVs)在这份名单上名列前茅,但家庭和工作场所接触均未与可检测到的血清学反应相关联。血清因子对γ逆转录病毒的非特异性失活似乎不足以解释这些观察结果。为了进一步研究,我们探讨了原代和已建立的人类细胞系对FeLV-B(最可能的人畜共患病变体)的易感性。完全允许的感染在癌症衍生的细胞系中很常见,但也是未转化的角质形成细胞和肺成纤维细胞的一个特征。造血来源的细胞通常较不易被感染,并根据细胞内蛋白质表达和病毒粒子释放的高低形成不同的组。在原代人血单核细胞和一部分白血病细胞系中观察到了强烈的抑制作用。然而,逆转录和整合的早期步骤在非允许细胞中似乎并未受损。在部分允许的细胞中,FeLV-B发生了G→A超突变,具有主要的载脂蛋白B mRNA编辑酶催化多肽样3G(APOBEC3G)特征,但在允许细胞或阻断二次病毒传播的非允许细胞中未发生突变。保护原代人血细胞的独特细胞屏障可能在预防FeLV人畜共患病感染中起重要作用。全世界都存在家庭接触γ逆转录病毒(如猫白血病病毒(FeLVs))的情况,但人类对感染的抵抗力基础仍未完全了解。从人类基因组序列中可以明显看出潜在威胁,该序列揭示了许多过去γ逆转录病毒感染的疫情,以及最近γ逆转录病毒从啮齿动物到灵长类动物和有袋动物的跨物种跳跃。本研究使用最常见的嗜人细胞FeLV变体FeLV-B在细胞水平上研究了对感染的抵抗力。我们发现,由于使病毒基因组发生突变的细胞酶的活性,血细胞对FeLV-B感染具有独特的抵抗力。还发现了第二个阻断机制,它似乎在病毒基因组整合到宿主细胞基因组后抑制病毒基因表达。由于来自其他正常人类细胞类型的细胞完全支持FeLV复制,血细胞的先天抵抗力可能在预防跨物种感染中起关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3a17/5309941/006c5b73e6c3/zjv9991823920001.jpg

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