Margolis Todd P, Elfman Fred L, Leib David, Pakpour Nazzy, Apakupakul Kathleen, Imai Yumi, Voytek Cindy
Francis I. Proctor Foundation, UCSF, Medical Sciences Building S-310, 513 Parnassus Ave., San Francisco, CA 94143-0412, USA.
J Virol. 2007 Oct;81(20):11069-74. doi: 10.1128/JVI.00243-07. Epub 2007 Aug 8.
Careful studies of mouse trigeminal ganglia (TG) latently infected with herpes simplex virus type 1 (HSV-1) indicate the presence of productive cycle viral gene products and persistent immune response, suggesting ongoing spontaneous viral reactivation in these tissues. In the present study we set out to determine whether infectious virus is present in murine TG latently infected with HSV-1 (KOS). At 37 days after ocular inoculation we found a small amount of infectious virus in ca. 6% of latently infected murine TG. Furthermore, the amount of infectious virus that we detected (PFU per viral antigen-positive neuron) was similar to that detected in acutely infected ganglia. We conclude that spontaneous reactivation of infectious HSV-1 occurs in the mouse TG and is likely the principle cause of viral protein expression in these tissues. We next examined the role of latency-associated transcript (LAT) in spontaneous ganglionic reactivation by examining ganglia latently infected with KOS dlLAT1.8, a LAT deletion virus. Through the use of immunocytochemistry we found that KOS dlLAT1.8 had a rate of spontaneous ganglionic reactivation very similar to that of HSV-1 (KOS). Studying spontaneous ganglionic reactivation of HSV in the mouse TG allows a direct study of viral reactivation from latently infected neurons without the potential confounders and complicating downstream events that accompany the study of viral reactivation by explantation or peripheral viral shedding. Since most cases of human viral shedding and reactivation are not associated with a known trigger, spontaneous ganglionic reactivation of HSV-1 may be a better model of human disease than existing models.
对感染1型单纯疱疹病毒(HSV-1)的小鼠三叉神经节(TG)进行的仔细研究表明,存在生产性周期病毒基因产物和持续的免疫反应,这表明这些组织中正在进行自发性病毒再激活。在本研究中,我们着手确定感染性病毒是否存在于潜伏感染HSV-1(KOS)的小鼠TG中。眼内接种后37天,我们在约6%的潜伏感染小鼠TG中发现了少量感染性病毒。此外,我们检测到的感染性病毒量(每个病毒抗原阳性神经元的空斑形成单位)与在急性感染神经节中检测到的量相似。我们得出结论,感染性HSV-1在小鼠TG中发生自发性再激活,并且可能是这些组织中病毒蛋白表达的主要原因。接下来,我们通过检查潜伏感染KOS dlLAT1.8(一种LAT缺失病毒)的神经节,研究了潜伏相关转录本(LAT)在神经节自发性再激活中的作用。通过免疫细胞化学方法,我们发现KOS dlLAT1.8的神经节自发性再激活率与HSV-1(KOS)非常相似。研究小鼠TG中HSV的神经节自发性再激活,可以直接研究潜伏感染神经元的病毒再激活,而不会受到外植法或外周病毒脱落研究病毒再激活时潜在的混杂因素和复杂的下游事件的影响。由于大多数人类病毒脱落和再激活病例与已知的触发因素无关,HSV-1的神经节自发性再激活可能比现有模型更适合作为人类疾病的模型。