Abstract
Herpes simplex virus 1 and 2 (HSV-1/2) similarly initiate infection in mucosal epithelia and establish lifelong neuronal latency. Anogenital HSV-2 infection augments the risk for sexual human immunodeficiency virus (HIV) transmission and is associated with higher HIV viral loads. However, whether oral HSV-1 infection contributes to oral HIV susceptibility, viremia, or oral complications of HIV infection is unknown. Appropriate non-human primate (NHP) models would facilitate this investigation, yet there are no published studies of HSV-1/SIV co-infection in NHPs. Thus, we performed a pilot study for an oral HSV-1 infection model in SIV-infected rhesus macaques to describe the feasibility of the modeling and resultant immunological changes. Three SIV-infected, clinically healthy macaques became HSV-1-infected by inoculation with 4 × 108 pfu HSV-1 McKrae on buccal, tongue, gingiva, and tonsils after gentle abrasion. HSV-1 DNA was shed in oral swabs for up to 21 days, and shedding recurred in association with intra-oral lesions after periods of no shedding during 56 days of follow up. HSV-1 DNA was detected in explant cultures of trigeminal ganglia collected at euthanasia on day 56. In the macaque with lowest baseline SIV viremia, SIV plasma RNA increased following HSV-1 infection. One macaque exhibited an acute pro-inflammatory response, and all three animals experienced T cell activation and mobilization in blood. However, T cell and antibody responses to HSV-1 were low and atypical. Through rigorous assessesments, this study finds that the virulent HSV-1 strain McKrae resulted in a low level HSV-1 infection that elicited modest immune responses and transiently modulated SIV infection.
Highlights
Herpes simplex virus (HSV) types 1 and 2 (HSV-1, HSV-2) are closely related alphaherpesviruses (Roizman et al, 2007)
Infection with HSV-1 is ubiquitous in humans; more than 50% of adults in the US are HSV-1 seropositive, and close to 100% are infected in some parts of the developing world (Looker et al, 2015)
Five adult female Indian rhesus macaques (Macaca mulatta; mean age: 10 years, range: 6–15 years; mean weight: 7.2 kg, range: 5.4–10.0 kg) that tested negative by serology for simian retrovirus (SRV), Herpes virus B, and simian T cell leukemia virus type 1 (STLV-1) were selected for these studies
Summary
Herpes simplex virus (HSV) types 1 and 2 (HSV-1, HSV-2) are closely related alphaherpesviruses (Roizman et al, 2007). HSV-1 typically initiates a productive lytic infection in the oral mucosal epithelium and establishes latency in the trigeminal ganglia after infecting sensory nerve termini adjacent to the site of mucosal virus replication. Infection with HSV-1 is ubiquitous in humans; more than 50% of adults in the US are HSV-1 seropositive, and close to 100% are infected in some parts of the developing world (Looker et al, 2015). Most HSV-1 infections are oral genital HSV-1 infection is on the rise, especially in the US and Europe (Looker et al, 2015). HSV-1 infection can lead to corneal HSV keratitis, representing the most common cause of infection-related blindness worldwide, and rarely encephalitis in adults and children
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