Attenuation of multiple Nef functions in HIV-1 elite controllers.

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dc.contributor.author Mwimanzi1,Philip
dc.date.accessioned 2013-04-22T06:42:25Z
dc.date.available 2013-04-22T06:42:25Z
dc.date.issued 2013
dc.identifier.citation Mwimanzi, P., Markle, T. J., Martin, E., Ogata, Y., Kuang, X. T., Tokunaga, M., ... & Ueno, T. (2013). Attenuation of multiple Nef functions in HIV-1 elite controllers. Retrovirology, 10(1), 1.
dc.identifier.other doi: 10.1186/1742-4690-10-1.
dc.identifier.uri http://hdl.handle.net/123456789/909
dc.description.abstract Abstract Background: Impaired HIV-1 Gag, Pol, and Env function has been described in elite controllers (EC) who spontaneously suppress plasma viremia to < 50 RNA copies/mL; however, activity of the accessory protein Nef remains incompletely characterized. We examined the ability of 91 Nef clones, isolated from plasma of 45 EC and 46 chronic progressors (CP), to down-regulate HLA class I and CD4, up-regulate HLA class II invariant chain (CD74), enhance viral infectivity, and stimulate viral replication in PBMC. Results: In general, EC Nef clones were functional; however, all five activities were significantly lower in EC compared to CP. Nef clones from HLA-B*57-expressing EC exhibited poorer CD4 down-regulation function compared to those from non-B*57 EC, and the number of EC-specific B*57-associated Nef polymorphisms correlated inversely with 4 of 5 Nef functions in these individuals. Conclusion: Results indicate that decreased HIV-1 Nef function, due in part to host immune selection pressures, may be a hallmark of the EC phenotype. en_GB
dc.language.iso en en_GB
dc.relation.ispartofseries Retrovirology. 10:1
dc.subject HIV-1, en_GB
dc.subject Nef, en_GB
dc.subject Immune escape, en_GB
dc.subject Human Leukocyte Antigen (HLA) class I, en_GB
dc.title Attenuation of multiple Nef functions in HIV-1 elite controllers. en_GB
dc.type Article en_GB


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