| Literature DB >> 10371501 |
T R Reddy1, W Xu, J K Mau, C D Goodwin, M Suhasini, H Tang, K Frimpong, D W Rose, F Wong-Staal.
Abstract
The HIV-1 Rev protein facilitates the nuclear export of mRNA containing the Rev response element (RRE) through binding to the export receptor CRM-1. Here we show that a cellular nuclear protein, Sam68 (Src-associated protein in mitosis), specifically interacts with RRE and can partially substitute for as well as synergize with Rev in RRE-mediated gene expression and virus replication. Differential sensitivity to leptomycin B, an inhibitor of CRM-1, indicates that the export pathways mediated by Rev and Sam68 are distinct. C-terminally deleted mutants of Sam68 inhibited the transactivation of RRE-mediated expression by both wild-type Sam68 and Rev. They were retained in the cytoplasm and impeded the nuclear localization of Rev in co-expressed cells. These mutants also inhibited wild-type HIV-1 replication to the same extent as the RevM10 mutant, and may be useful as anti-viral agents in the treatment of AIDS.Entities:
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Year: 1999 PMID: 10371501 DOI: 10.1038/9479
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440