Transactive Response DNA- Binding Protein (TARDBP/TDP-43) Regulates Cell Permissivity to HIV- 1 Infection by Acting on HDAC6.
Autor
Valenzuela Fernández, Agustín; Cabrera Rodríguez, Romina; Pérez Yanes, Silvia; Montelongo, Rafaela; Lorenzo Salazar, José M.; Estévez Herrera, Judith; García Luis, Jonay; Íñigo Campos, Antonio; Rubio Rodríguez, Luis A.; Muñoz Barrera, Adrián; Trujillo González, Rodrigo Francisco; Dorta Guerra, Roberto; Casado, Concha; Pernas, María; Blanco, Julià; Flores, CarlosFecha
2022Resumen
The transactive response DNA-binding protein (TARDBP/TDP-43) influences the processing of diverse transcripts, including that of histone deacetylase 6 (HDAC6). Here, we assessed TDP-43
activity in terms of regulating CD4+ T-cell permissivity to HIV-1 infection. We observed that overexpression of wt-TDP-43 increased both mRNA and protein levels of HDAC6, resulting in impaired
HIV-1 infection independently of the viral envelope glycoprotein complex (Env) tropism. Consistently, using an HIV-1 Env-mediated cell-to-cell fusion model, the overexpression of TDP-43 levels
negatively affected viral Env fusion capacity. Silencing of endogenous TDP-43 significantly decreased
HDAC6 levels and increased the fusogenic and infection activities of the HIV-1 Env. Using pseudovirus bearing primary viral Envs from HIV-1 individuals, overexpression of wt-TDP-43 strongly
reduced the infection activity of Envs from viremic non-progressors (VNP) and rapid progressors
(RP) patients down to the levels of the inefficient HIV-1 Envs observed in long-term non-progressor
elite controllers (LTNP-EC). On the contrary, silencing endogenous TDP-43 significantly favored the
infectivity of primary Envs from VNP and RP individuals, and notably increased the infection of
those from LTNP-EC. Taken together, our results indicate that TDP-43 shapes cell permissivity to
HIV-1 infection, affecting viral Env fusion and infection capacities by altering the HDAC6 levels and
associated tubulin-deacetylase anti-HIV-1 activity