2010
DOI: 10.1007/s00430-010-0158-x
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Molecular biology of foamy viruses

Abstract: One of the most fascinating areas in retrovirology is the study of foamy viruses (FVs), because these viruses appear to do everything that is common to all other retroviruses differently. FVs have found a completely new way to propagate their genome. And they do this extremely successfully because most of wild non-human primates, felines, bovines, equines, and small ruminants are likely to be non-pathogenically infected. The success of FVs can also be viewed from a different angle, since they replicate very co… Show more

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Cited by 56 publications
(82 citation statements)
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References 111 publications
(144 reference statements)
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“…imian foamy viruses (SFVs) belong in the Spumavirus genus of the Spumaretrovirinae subfamily of Retroviridae and are widespread in all nonhuman primates (NHPs) (1,2). SFVs have been isolated from various tissues of different NHPs and were originally designated based upon neutralization serotyping (3).…”
mentioning
confidence: 99%
“…imian foamy viruses (SFVs) belong in the Spumavirus genus of the Spumaretrovirinae subfamily of Retroviridae and are widespread in all nonhuman primates (NHPs) (1,2). SFVs have been isolated from various tissues of different NHPs and were originally designated based upon neutralization serotyping (3).…”
mentioning
confidence: 99%
“…The actual details of this mechanism are still largely unknown. However, it appears to be linked to the packaging of another essential component of the infectious viral particle, the viral genomic RNA (29,32). Current data suggest that protein-RNA interaction of both Gag and Pol with viral genomic RNA as well as protein-protein interactions between Gag and Pol are involved in the assembly process (14,21,29).…”
mentioning
confidence: 99%
“…For the Gag proteins of nonprimate FVs, feline FV (FFV), bovine FV (BFV), and equine FV (EFV), no clustering of GR residues is observed, and only small peptide motifs of GR box II (GRII) and GR box III (GRIII) are conserved throughout all FV Gag proteins (25,35,42,43). The GR-rich FV Gag C terminus and, in particular, the clustered GR boxes of primate FVs are thought to play roles in viral replication similar to those of the Cys-His motifs of orthoretroviruses (32).…”
mentioning
confidence: 99%
“…FV replication involves several unique characteristics that distinguish these viruses from the orthoretroviruses (5). An important difference is the expression of FV Pol as a separate precursor protein from a singly spliced mRNA and not as a Gag-Pol fusion protein from unspliced viral genomic RNA (6,7).…”
mentioning
confidence: 99%
“…An important difference is the expression of FV Pol as a separate precursor protein from a singly spliced mRNA and not as a Gag-Pol fusion protein from unspliced viral genomic RNA (6,7). Thus, the FV Pol precursor cannot be packaged into newly forming capsids in an orthoretroviral-like fashion as part of a Gag-Pol fusion protein; instead, FVs directly incorporate the Pol protein into assembling virions (5). Although the mechanism of FV Pol encapsidation is only partially understood, it seems clear that viral RNA (vRNA) is necessary for efficient prototype FV (PFV) Pol particle incorporation (8)(9)(10).…”
mentioning
confidence: 99%