Yang L, Voytek C C, Margolis T P
F. I. Proctor Foundation and Department of Ophthalmology, University of California, San Francisco, San Francisco, California 94143-0944, USA.
J Virol. 2000 Jan;74(1):209-17. doi: 10.1128/jvi.74.1.209-217.2000.
We characterized the populations of primary sensory neurons that become latently infected with herpes simplex virus (HSV) following peripheral inoculation. Twenty-one days after ocular inoculation with HSV strain KOS, 81% of latency-associated transcript (LAT)-positive trigeminal ganglion (TG) neurons coexpressed SSEA3, 71% coexpressed Trk(A) (the high-affinity nerve growth factor receptor), and 68% coexpressed antigen recognized by monoclonal antibody (MAb) A5; less than 5% coexpressed antigen recognized by MAb KH10. The distribution of LAT-positive, latently infected TG neurons contrasted sharply with (i) the overall distribution of neuronal phenotypes in latently infected TG and (ii) the neuronal distribution of viral antigen in productively infected TG. Similar results were obtained following ocular and footpad inoculation with KOS/62, a LAT deletion mutant in which the LAT promoter is used to drive expression of the Escherichia coli lacZ gene. Thus, although all neuronal populations within primary sensory ganglia appear to be capable of supporting a productive infection with HSV, some neuronal phenotypes are more permissive for establishment of a latent infection with LAT expression than others. Furthermore, expression of HSV LAT does not appear to play a role in this process. These findings indicate that there are marked differences in the outcome of HSV infection among the different neuronal populations in the TG and highlight the key role that the host neuron may play in regulating the repertoire of viral gene expression during the establishment of HSV latent infection.
我们对在周围接种后潜伏感染单纯疱疹病毒(HSV)的初级感觉神经元群体进行了特征描述。用HSV毒株KOS进行眼部接种21天后,81%的潜伏相关转录本(LAT)阳性三叉神经节(TG)神经元共表达阶段特异性胚胎抗原3(SSEA3),71%共表达酪氨酸激酶A(Trk(A),高亲和力神经生长因子受体),68%共表达单克隆抗体(MAb)A5识别的抗原;共表达MAb KH10识别的抗原的神经元不到5%。LAT阳性、潜伏感染的TG神经元的分布与(i)潜伏感染的TG中神经元表型的总体分布以及(ii)有 productive感染的TG中病毒抗原的神经元分布形成鲜明对比。在用KOS/62进行眼部和足垫接种后也得到了类似结果,KOS/62是一种LAT缺失突变体,其中LAT启动子用于驱动大肠杆菌lacZ基因的表达。因此,尽管初级感觉神经节内的所有神经元群体似乎都能够支持HSV的 productive感染,但某些神经元表型比其他表型更易于建立具有LAT表达的潜伏感染。此外,HSV LAT的表达似乎在这一过程中不起作用。这些发现表明,TG中不同神经元群体之间HSV感染的结果存在显著差异,并突出了宿主神经元在HSV潜伏感染建立过程中调节病毒基因表达谱方面可能发挥的关键作用。