| Literature DB >> 16148047 |
Agustín Valenzuela-Fernández1, Susana Alvarez, Mónica Gordon-Alonso, Marta Barrero, Angeles Ursa, J Román Cabrero, Gerónimo Fernández, Salvador Naranjo-Suárez, Maria Yáñez-Mo, Juan M Serrador, M Angeles Muñoz-Fernández, Francisco Sánchez-Madrid.
Abstract
Efficient human immunodeficiency virus (HIV)-1 infection depends on multiple interactions between the viral gp41/gp120 envelope (Env) proteins and cell surface receptors. However, cytoskeleton-associated proteins that modify membrane dynamics may also regulate the formation of the HIV-mediated fusion pore and hence viral infection. Because the effects of HDAC6-tubulin deacetylase on cortical alpha-tubulin regulate cell migration and immune synapse organization, we explored the possible role of HDAC6 in HIV-1-envelope-mediated cell fusion and infection. The binding of the gp120 protein to CD4+-permissive cells increased the level of acetylated alpha-tubulin in a CD4-dependent manner. Furthermore, overexpression of active HDAC6 inhibited the acetylation of alpha-tubulin, and remarkably, prevented HIV-1 envelope-dependent cell fusion and infection without affecting the expression and codistribution of HIV-1 receptors. In contrast, knockdown of HDAC6 expression or inhibition of its tubulin deacetylase activity strongly enhanced HIV-1 infection and syncytia formation. These results demonstrate that HDAC6 plays a significant role in regulating HIV-1 infection and Env-mediated syncytia formation.Entities:
Mesh:
Substances:
Year: 2005 PMID: 16148047 PMCID: PMC1266439 DOI: 10.1091/mbc.e05-04-0354
Source DB: PubMed Journal: Mol Biol Cell ISSN: 1059-1524 Impact factor: 4.138