Nef defect attenuates HIV viremia and immune dysregulation in the bone marrow-liver-thymus-spleen (BLTS) humanized mouse model.
Shivkumar BiradarYash AgarwalAntu DasSherry T ShuJasmine SamalSara HoNickolas KellyDeepika MaheshShreya TeredesaiIsabella CastronovaLondon MussinaRobbie B MailliardThomas E SmithgallMoses T BilityPublished in: Virology (2024)
In vitro studies have shown that deletion of nef and deleterious mutation in the Nef dimerization interface attenuates HIV replication and associated pathogenesis. Humanized rodents with human immune cells and lymphoid tissues are robust in vivo models for investigating the interactions between HIV and the human immune system. Here, we demonstrate that nef deletion impairs HIV replication and HIV-induced immune dysregulation in the blood and human secondary lymphoid tissue (human spleen) in bone marrow-liver-thymus-spleen (BLTS) humanized mice. Furthermore, we also show that nef defects (via deleterious mutations in the dimerization interface) impair HIV replication and HIV-induced immune dysregulation in the blood and human spleen in BLTS-humanized mice. We demonstrate that the reduced replication of nef-deleted and nef-defective HIV is associated with robust antiviral innate immune response, and T helper 1 response. Our results support the proposition that Nef may be a therapeutic target for adjuvants in HIV cure strategies.
Keyphrases
- antiretroviral therapy
- hiv positive
- hiv infected
- hiv testing
- human immunodeficiency virus
- hepatitis c virus
- hiv aids
- endothelial cells
- men who have sex with men
- immune response
- bone marrow
- south africa
- high glucose
- induced pluripotent stem cells
- type diabetes
- dendritic cells
- monoclonal antibody
- oxidative stress
- skeletal muscle
- metabolic syndrome
- high fat diet induced