| Literature DB >> 29594984 |
Sanjeev Gumber1, Praveen Kumar Amancha2, Po-Jen Yen3, Francois Villinger2, Dana Gabuzda3, Siddappa N Byrareddy4.
Abstract
Macrophages are a major target of HIV/SIV infection and play an important role in pathogenesis by serving as viral reservoirs in the central nervous system. Previously, a unique early SIVmac251 envelope (Env) variant, deSIV147 was cloned from blood of a rhesus macaque with rapid disease progression and SIV-associated encephalitis. Here, we show that infectious molecular clone deSIV147 caused systemic infection in rhesus macaques following intravenous or intrarectal exposure. Next, we inoculated deSIV147 into macaques depleted of CD4+ T cells and found that animals were SIV-positive, with high plasma and CSF viral loads. These macaques also showed SIVp17-positive macrophages in brain, lymph nodes, colon, lung, and liver. Furthermore, accumulation of perivascular macrophages, multinucleated giant cells, and microgliosis was detected. These findings suggest that the neurotropic deSIV147 clone will be useful to study macrophage infection in HIV/SIV-associated neurocognitive disorders, gain insights into myeloid cell reservoirs in brain and other anatomical sites, as well as test strategies for eradication.Entities:
Keywords: Central nerveous system; Macrophage-tropic; Macrophages; Myeloid cells; Rhesus macaques; SIV
Mesh:
Year: 2018 PMID: 29594984 PMCID: PMC6105460 DOI: 10.1007/s13365-018-0628-2
Source DB: PubMed Journal: J Neurovirol ISSN: 1355-0284 Impact factor: 2.643