1996
DOI: 10.1128/jvi.70.2.1016-1026.1996
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Evidence for a second function of the MA sequence in the Rous sarcoma virus Gag protein

Abstract: During retrovirus assembly, Gag proteins bind to the inner leaflet of the plasma membrane to initiate the budding process. The molecular basis of this protein-lipid interaction is poorly understood. For the human immunodeficiency virus type 1 Gag protein, we recently reported that the membrane-binding domain resides within the N-terminal 31 amino acids and consists of two components: myristate and a cluster of basic residues, which together promote membrane binding in vitro and budding in vivo (W. Zhou, L. J. … Show more

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Cited by 52 publications
(24 citation statements)
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“…The low level of particle release exhibited by this mutant cannot explain the loss of infectivity, since the EP peptide restored infectivity despite further decreasing the budding efficiency. Moreover, independent studies in our laboratory have revealed additional MA mutants that are noninfectious even though they produce wild-type levels of particles (27). Hence, these studies provide evidence for an additional function for the MA protein of RSV.…”
Section: Discussionmentioning
confidence: 66%
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“…The low level of particle release exhibited by this mutant cannot explain the loss of infectivity, since the EP peptide restored infectivity despite further decreasing the budding efficiency. Moreover, independent studies in our laboratory have revealed additional MA mutants that are noninfectious even though they produce wild-type levels of particles (27). Hence, these studies provide evidence for an additional function for the MA protein of RSV.…”
Section: Discussionmentioning
confidence: 66%
“…Functional equivalents of these assembly domains have been found in the Gag proteins of unrelated retroviruses, including those of human im-munodeficiency virus (HIV) and murine leukemia virus. Moreover, these heterologous sequences can fully replace the RSV assembly functions in spite of their lack of sequence similarity (2,21,26,27).…”
mentioning
confidence: 99%
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“…One previous study showed that the second half of the MA protein of the oncoretrovirus RSV is dispensable for viral infectivity (Nelle and Wills, 1996). However, even small alterations in the N-terminal half of RSV MA completely abolished virus budding or infectivity (Nelle and Wills, 1996;Parent et al, 1996). In the case of HIV-1, relatively subtle alterations in MA often had drastic effects on HIV-1 morphogenesis and infectivity.…”
Section: Discussionmentioning
confidence: 99%
“…for the N-terminal 100 residues of ASV Gag for budding of VLPs and weakly substitute for the N-terminal 10 residues (40). The N-terminal 32 residues of HIV-1 Gag contain three membrane-binding signals: the myr group, the conserved basic region, and a PI(4,5)P 2 -binding pocket (41,42).…”
Section: Determinants Of Asv Gag Plasma Membrane Targetingmentioning
confidence: 99%