Biological activity of human immunodeficiency virus type 1 Vif requires membrane targeting by C-terminal basic domains

Goncalves, J; Shi, Bin; Yang, Xinzhen; Gabuzda, Dana

doi:10.1128/jvi.69.11.7196-7204.1995

Cited by 62 publications

(45 citation statements)

References 44 publications

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“…4 and 5). It has also been reported that the combined action of a number of positively charged amino acids toward Vif's carboxy terminus contributes to function (2,11,13). Although the substitution of the lysines at positions 157 and 160 had no effect on activity (Fig.…”

Section: Discussionmentioning

confidence: 84%

Mutational Analysis of the Human Immunodeficiency Virus Type 1 Vif Protein

Simon¹,

Sheehy

Carpenter

et al. 1999

J Virol

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Lentivirus Vif proteins are potent regulators of virus infectivity. However, relatively little is known about the functional domains, peptide motifs, or residues of any Vif protein. In this report, we present the first extensive mutagenesis analysis of the 192-amino-acid human immunodeficiency virus type 1 (HIV-1) Vif protein. A large number of scanning missense (mostly alanine substitution) and deletion mutations were introduced into the HIV-1HXB3 vif gene, and the resulting proteins were evaluated for the induction of virus infectivity as well as subcellular localization. The results show that amino acids dispersed throughout Vif’s linear sequence are important for function. However, because many of the inactive proteins also appear to be mislocalized, we suggest that many of them may actually be misfolded rather lacking an intracellular targeting signal. Interestingly, disruptions within an internal region spanning residues 114 to 146 give rise to mutant proteins that either retain function or are inactive but are not substantially mislocalized. We therefore speculate that this region, which harbors two essential cysteine residues and one essential serine residue, may contain aspects of a putative Vif effector domain.

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Section: Discussionmentioning

confidence: 84%

Mutational Analysis of the Human Immunodeficiency Virus Type 1 Vif Protein

Simon¹,

Sheehy

Carpenter

et al. 1999

J Virol

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“…Between these regions, conserved motifs were observed, in particular the SLQXLA motif located between amino acids 144 and 149 (Oberste and Gonda, 1992) and two other motifs in the last 30 C-terminal amino acids of the Vif protein, i.e., 161 PPLPS 165 and 168 KLTEDRWN 175 . These two latter motifs are located in the domain which is in association with the plasma membrane and with the Gagprecursor (Bouyac et al, 1997;Goncalves et al, 1995). Moreover Arg and Lys residues within the C-terminal end of Vif (8 to 11 residues between the positions 157 and 192), which are the most important residues for those interactions, are largely conserved in all LTNP as well as in late progressor Vif sequences.…”

Section: Definition Of the Asymptomatic Subjectsmentioning

confidence: 99%

Characterization of Human Immunodeficiency Virus Type 1 vif Gene in Long-Term Asymptomatic Individuals

et al. 2000

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We have determined the sequence of the human immunodeficiency virus type 1 (HIV-1) vif genes from a cohort of 42 long-term nonprogressors (LTNP) and compared these sequences to those of 8 late progressors. The coding potential of the vif open reading frame directly derived by nested PCR from uncultured peripheral blood mononuclear cell DNA was conserved in all 50 individuals. The nucleotide distances between vif sequences were not significantly different between LTNP and late progressors, indicating similar selections of viruses within both types of long-term HIV-1-infected subjects. However, a statistically significant correlation between an amino acid signature at position 132 of Vif and the viral load was found within LTNP. Namely, amino acid Ser was associated with low viral load and amino acid Arg with high viral load. This signature was also observed when LTNP with low viral load were compared to progressors. The Ser132 signature was introduced in place of Arg132 present in the HIV-1 YU-2 Vif prototype into chimeric viruses to assess the impact of Vif signature on the virus. While the replication properties in the SupT1 cell line were unmodified, the mutagenized virus revealed a fivefold decreased replication in activated PBMC, suggesting a possible role of this Vif signature for viral production in vivo.

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“…Nevertheless, it was suggested that Vif is required at the time of particle production in the host cell for regulating virus assembly or maturation (2,3,11,35,49). Vif has been shown to associate with the cytoplasmic face of cellular membranes (17), a phenomenon that involves basic residues located in the C-terminal portion of Vif (18). Vif muta-tions that disrupt membrane association also affect Vif function (18), suggesting a correlation between membrane binding and Vif activity.…”

Section: The Human Immunodeficiency Virus Type 1 (Hiv-1) Vif Protein mentioning

confidence: 99%

“…Vif has been shown to associate with the cytoplasmic face of cellular membranes (17), a phenomenon that involves basic residues located in the C-terminal portion of Vif (18). Vif muta-tions that disrupt membrane association also affect Vif function (18), suggesting a correlation between membrane binding and Vif activity.…”

Section: The Human Immunodeficiency Virus Type 1 (Hiv-1) Vif Protein mentioning

confidence: 99%

“…We therefore conclude that the partitioning of Vif with the cytoskeletal fraction is not due to nonspecific aggregation of Vif but is an inherent feature of this viral protein and most likely reflects the association of Vif with cytoskeletal components. It should be noted that previous studies investigating the subcellular distribution of Vif reported a significant amount of Vif associated with cellular membranes (17,18,32). However, these studies did not analyze cytoskeletal fractions of cells and thus ignored the portion of Vif that partitions with that fraction.…”

Section: Cytoskeleton Association Of Vif It Was Recently Reported Thatmentioning

confidence: 99%

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Cytoskeleton association and virion incorporation of the human immunodeficiency virus type 1 Vif protein

Karczewski

Strebel

1996

J Virol

142

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The human immunodeficiency virus type 1 (HIV-1) Vif protein has an important role in the regulation of virus infectivity. This function of Vif is cell type specific, and virions produced in the absence of Vif in restrictive cells have greatly reduced infectivity. We show here that the intracellular localization of Vif is dependent on the presence of the intermediate filament vimentin. Fractionation of acutely infected T cells or transiently transfected HeLa cells demonstrates the existence of a soluble and a cytoskeletal form and to a lesser extent the presence of a detergent-extractable form of Vif. Confocal microscopy suggests that in HeLa cells, Vif is predominantly present in the cytoplasm and closely colocalizes with the intermediate filament vimentin. Treatment of cells with drugs affecting the structure of vimentin filaments affect the localization of Vif accordingly, indicating a close association of Vif with this cytoskeletal component. The association of Vif with vimentin can cause the collapse of the intermediate filament network into a perinuclear aggregate. In contrast, analysis of Vif in vimentin-negative cells reveals significant staining of the nucleus and the nuclear membrane in addition to diffuse cytoplasmic staining. In addition to the association of Vif with intermediate filaments, analyses of virion preparations demonstrate that Vif is incorporated into virus particles. In sucrose density gradients, Vif cosediments with capsid proteins even after detergent treatment of virus preparations, suggesting that Vif is associated with the inner core of HIV particles. We propose a model in which Vif has a crucial function as a virion component either by regulating virus maturation or following virus entry into a host cell possibly involving an interaction with the cellular cytoskeletal network.

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Biological activity of human immunodeficiency virus type 1 Vif requires membrane targeting by C-terminal basic domains

Cited by 62 publications

References 44 publications

Mutational Analysis of the Human Immunodeficiency Virus Type 1 Vif Protein

Mutational Analysis of the Human Immunodeficiency Virus Type 1 Vif Protein

Characterization of Human Immunodeficiency Virus Type 1 vif Gene in Long-Term Asymptomatic Individuals

Cytoskeleton association and virion incorporation of the human immunodeficiency virus type 1 Vif protein

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