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Abstract
BackgroundMouse mammary tumor virus (MMTV) encodes the Rem protein, an HIV Rev-like protein that enhances nuclear export of unspliced viral RNA in rodent cells. We have shown that Rem is expressed from a doubly spliced RNA, typical of complex retroviruses. Several recent reports indicate that MMTV can infect human cells, suggesting that MMTV might interact with human retroviruses, such as human immunodeficiency virus (HIV), human T-cell leukemia virus (HTLV), and human endogenous retrovirus type K (HERV-K). In this report, we test whether the export/regulatory proteins of human complex retroviruses will increase expression from vectors containing the Rem-responsive element (RmRE).ResultsMMTV Rem, HIV Rev, and HTLV Rex proteins, but not HERV-K Rec, enhanced expression from an MMTV-based reporter plasmid in human T cells, and this activity was dependent on the RmRE. No RmRE-dependent reporter gene expression was detectable using Rev, Rex, or Rec in HC11 mouse mammary cells. Cell fractionation and RNA quantitation experiments suggested that the regulatory proteins did not affect RNA stability or nuclear export in the MMTV reporter system. Rem had no demonstrable activity on export elements from HIV, HTLV, or HERV-K. Similar to the Rem-specific activity in rodent cells, the RmRE-dependent functions of Rem, Rev, or Rex in human cells were inhibited by a dominant-negative truncated nucleoporin that acts in the Crm1 pathway of RNA and protein export.ConclusionThese data argue that many retroviral regulatory proteins recognize similar complex RNA structures, which may depend on the presence of cell-type specific proteins. Retroviral protein activity on the RmRE appears to affect a post-export function of the reporter RNA. Our results provide additional evidence that MMTV is a complex retrovirus with the potential for viral interactions in human cells.
Highlights
Mouse mammary tumor virus (MMTV) encodes the Rem protein, an human immunodeficiency virus (HIV) Rev-like protein that enhances nuclear export of unspliced viral RNA in rodent cells
To determine if the RNA export proteins from known complex retroviruses function on the MMTV Rem-responsive element (RmRE), we used the reporter vector, pHMRluc (Figure 1) [5]
Rem expression gave a 25 to 30-fold increase in luciferase expression in Jurkat human T cells relative to cells co-transfected with the reporter plasmid and empty vector, whereas no increase was observed using the reporter lacking a functional RmRE (Figure 2A)
Summary
Mouse mammary tumor virus (MMTV) encodes the Rem protein, an HIV Rev-like protein that enhances nuclear export of unspliced viral RNA in rodent cells. The. N-terminal portion of Rem contains nuclear and nucleolar localization signals as well as an arginine-rich motif similar to the RNA export proteins, Rev, Rex, and Rec, produced by the complex retroviruses, human immunodeficiency virus (HIV), human T-cell leukemia virus (HTLV), and human endogenous retrovirus type-K (page number not for citation purposes). Amplification of MMTV in various lymphoid cell types requires virally encoded Sag to effectively transfer virus from lymphocytes to mammary epithelial cells during puberty [12, 13]. Both the sophisticated mode of transmission and production of multiple accessory and regulatory proteins imply that MMTV is a complex retrovirus [5]
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