新生儿神经祖细胞及其神经元和神经胶质细胞衍生物对人巨细胞病毒感染完全易感。
Neonatal neural progenitor cells and their neuronal and glial cell derivatives are fully permissive for human cytomegalovirus infection.
作者信息
Luo Min Hua, Schwartz Philip H, Fortunato Elizabeth A
机构信息
Department of Microbiology, Molecular Biology and Biochemistry and the Center for Reproductive Biology, University of Idaho, Moscow, ID 83844-3052, USA.
出版信息
J Virol. 2008 Oct;82(20):9994-10007. doi: 10.1128/JVI.00943-08. Epub 2008 Aug 6.
Congenital human cytomegalovirus (HCMV) infection causes central nervous system structural abnormalities and functional disorders, affecting both astroglia and neurons with a pathogenesis that is only marginally understood. To better understand HCMV's interactions with such clinically important cell types, we utilized neural progenitor cells (NPCs) derived from neonatal autopsy tissue, which can be differentiated down either glial or neuronal pathways. Studies were performed using two viral isolates, Towne (laboratory adapted) and TR (a clinical strain), at a multiplicity of infection of 3. NPCs were fully permissive for both strains, expressing the full range of viral antigens (Ags) and producing relatively large numbers of infectious virions. NPCs infected with TR showed delayed development of cytopathic effects (CPE) and replication centers and shed less virus. This pattern of delay for TR infections held true for all cell types tested. Differentiation of NPCs was carried out for 21 days to obtain either astroglia (>95% GFAP(+)) or a 1:5 mixed neuron/astroglia population (beta-tubulin III(+)/GFAP(+)). We found that both of these differentiated populations were fully permissive for HCMV infection and produced substantial numbers of infectious virions. Utilizing a difference in plating efficiencies, we were able to enrich the neuron population to approximately 80% beta-tubulin III(+) cells. These beta-tubulin III(+)-enriched populations remained fully permissive for infection but were very slow to develop CPE. These infected enriched neurons survived longer than either NPCs or astroglia, and a small proportion were alive until at least 14 days postinfection. These surviving cells were all beta-tubulin III(+) and showed viral Ag expression. Surprisingly, some cells still exhibited extended processes, similar to mock-infected neurons. Our findings strongly suggest neurons as reservoirs for HCMV within the developing brain.
先天性人类巨细胞病毒(HCMV)感染会导致中枢神经系统结构异常和功能紊乱,影响星形胶质细胞和神经元,但其发病机制仍知之甚少。为了更好地理解HCMV与这些临床上重要的细胞类型之间的相互作用,我们利用了源自新生儿尸检组织的神经祖细胞(NPC),这些细胞可以分化为胶质细胞或神经元途径。研究使用了两种病毒分离株,Towne(实验室适应株)和TR(临床株),感染复数为3。NPC对这两种毒株均完全易感,表达全套病毒抗原(Ag)并产生相对大量的感染性病毒粒子。感染TR的NPC表现出细胞病变效应(CPE)和复制中心的发育延迟,且释放的病毒较少。TR感染的这种延迟模式在所有测试的细胞类型中均成立。NPC分化21天以获得星形胶质细胞(>95% GFAP(+))或1:5的混合神经元/星形胶质细胞群体(β-微管蛋白III(+)/GFAP(+))。我们发现这两种分化群体对HCMV感染均完全易感,并产生大量感染性病毒粒子。利用接种效率的差异,我们能够将神经元群体富集到约80%的β-微管蛋白III(+)细胞。这些富含β-微管蛋白III(+)的群体对感染仍完全易感,但CPE发展非常缓慢。这些感染的富集神经元比NPC或星形胶质细胞存活时间更长,一小部分至少在感染后14天仍存活。这些存活细胞均为β-微管蛋白III(+)并显示病毒Ag表达。令人惊讶的是,一些细胞仍表现出延长的突起,类似于 mock 感染的神经元。我们的发现强烈表明神经元是发育中大脑内HCMV的储存库。
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