HIV-1 subtype C with PYxE insertion has enhanced binding of Gag-p6 to host cell protein ALIX and increased replication fitness

Domselaar, Robert van; Njenda, Duncan; Rao, Rohit; Sönnerborg, Anders; Singh, Kulwant; Neogi, Ujjwal

doi:10.1101/459156

Cited by 3 publications

(8 citation statements)

References 40 publications

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“…It has been suggested that Gag can be in a compact conformational structure when in solution or an extended conformational structure when bound to the plasma membrane when still at the immature non-processed state, although these observations were demonstrated with Gag molecules that are lacking the P6 domain (29). Gag is predominantly localized at the plasma membrane (16,30,31), and the P6 domain plays an important role prior and during the virion assembly phase (15). Therefore, this domain is exposed to binding to other viral and host cell proteins and thus also exposed for targeting by GrM.…”

Section: Discussionmentioning

confidence: 99%

“…Therefore, this domain is exposed to binding to other viral and host cell proteins and thus also exposed for targeting by GrM. Even though only a relatively small 2 kDa C-terminal part of the P6 late domain is being cleaved off, this exposed domain is important for its interaction with host cell protein ALIX and serves as a binding domain for HIV-1 accessory protein Vpr (16,(32)(33)(34)(35)(36)(37). The GrM cleavage site is directly after the ALIX binding motif and cleavage could disturb the interaction of ALIX with Gag and thereby affecting the budding of virions from the plasma membrane (16,33).…”

Section: Discussionmentioning

confidence: 99%

“…Even though only a relatively small 2 kDa C-terminal part of the P6 late domain is being cleaved off, this exposed domain is important for its interaction with host cell protein ALIX and serves as a binding domain for HIV-1 accessory protein Vpr (16,(32)(33)(34)(35)(36)(37). The GrM cleavage site is directly after the ALIX binding motif and cleavage could disturb the interaction of ALIX with Gag and thereby affecting the budding of virions from the plasma membrane (16,33). The motif for binding Vpr to Gag, LXSLFG, is located after the GrM cleavage site and deletion of this motif completely abolishes the incorporation of Vpr into virions (32,(34)(35)(36)(37).…”

Section: Discussionmentioning

confidence: 99%

“…pCR3.1/HIV1B-Gag-mCherry (HIV-1B Gag) was a kind gift from Dr. Paul Bieniasz (The Rockefeller University, USA). pCR3.1/ HIV1C-Gag-mCherry variants with or without PYKE or PYQE tetrapeptide insertions were described previously (16). The Gag PYKEi-L483A mutant was generated by PCR-directed cloning using pCR3.1/HIV-GagPYKEi-mCherry as template.…”

Section: Plasmidsmentioning

confidence: 99%

“…The PYKE motif is important for the interaction of the viral Gag to host cell protein ALIX that facilitates viral budding. Furthermore, insertion of this motif correlated with enhanced viral fitness (16,17). Interestingly, HIV-1C Gag with the PYKE insertion (Gag PYKEi ) contains the GrM consensus substrate motif KEPL overlapping the PYKE motif, whereas HIV-1B and HIV-1C without the tetrapeptide insertion only contain the proline and leucine residues at this site within Gag.…”

Section: Introductionmentioning

confidence: 99%

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Cytotoxic Lymphocytes Target HIV-1 Gag Through Granzyme M-Mediated Cleavage

et al. 2021

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Untreated HIV-1 infection leads to a slow decrease in CD4+ T cell lymphocytes over time resulting in increased susceptibility to opportunistic infections (acquired immunodeficiency syndrome, AIDS) and ultimately death of the infected individual. Initially, the host’s immune response controls the infection, but cannot eliminate the HIV-1 from the host. Cytotoxic lymphocytes are the key effector cells in this response and can mediate crucial antiviral responses through the release of a set of proteases called granzymes towards HIV-1-infected cells. However, little is known about the immunological molecular mechanisms by which granzymes could control HIV-1. Since we noted that HIV-1 subtype C (HIV-1C) Gag with the tetrapeptide insertion PYKE contains a putative granzyme M (GrM) cleavage site (KEPL) that overlaps with the PYKE insertion, we analyzed the proteolytic activity of GrM towards Gag. Immunoblot analysis showed that GrM could cleave Gag proteins from HIV-1B and variants from HIV-1C of which the Gag-PYKE variant was cleaved with extremely high efficiency. The main cleavage site was directly after the insertion after leucine residue 483. GrM-mediated cleavage of Gag was also observed in co-cultures using cytotoxic lymphocytes as effector cells and this cleavage could be inhibited by a GrM inhibitor peptide. Altogether, our data indicate towards a noncytotoxic immunological mechanism by which GrM-positive cytotoxic lymphocytes target the HIV-1 Gag protein within infected cells to potentially control HIV-1 infection. This mechanism could be exploited in new therapeutic strategies to treat HIV-1-infected patients to improve immunological control of the infection.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Plasmidsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Cytotoxic Lymphocytes Target HIV-1 Gag Through Granzyme M-Mediated Cleavage

et al. 2021

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Cytotoxic lymphocytes target HIV-1 Gag through granzyme M-mediated cleavage

Saccon

Mikaeloff

Ivern

et al. 2021

Preprint

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HIV-1 leads to progression to immunodeficiency and death of individuals who do not receive successful antiretroviral therapy. Initially, the host its immune response controls the infection, but cannot eliminate the HIV-1 from the host. Cytotoxic lymphocytes are the key effector cells in this response and can mediate crucial antiviral responses through the release of a set of proteases called granzymes towards HIV-1-infected cells. However, little is known about the immunological molecular mechanisms by which granzymes could control HIV-1. Since we noted that HIV-1 subtype C (HIV-1C) Gag with the tetrapeptide insertion PYKE contains a putative granzyme M (GrM) cleavage site (KEPL) that overlaps with the PYKE insertion, we analyzed the proteolytic activity of GrM towards Gag. Immunoblot analysis showed that GrM could cleave Gag proteins from HIV-1B and variants from HIV-1C of which the Gag-PYKE variant was cleaved with extremely high efficiency. The main cleavage site was directly after the insertion after leucine residue 483. GrM-mediated cleavage of Gag was also observed in co-cultures using cytotoxic lymphocytes as effector cells and this cleavage could be inhibited by a GrM inhibitor peptide. Altogether, our data indicate towards a noncytotoxic immunological mechanism by which GrM-positive cytotoxic lymphocytes target the HIV-1 Gag protein within infected cells to potentially control HIV-1 infection. This mechanism could be exploited in new therapeutic strategies to treat HIV-1-infected patients to improve immunological control of the infection.

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HIV-1 Subtype C with PYxE Insertion Has Enhanced Binding of Gag-p6 to Host Cell Protein ALIX and Increased Replication Fitness

Domselaar

Njenda

Rao

et al. 2019

J Virol

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Human immunodeficiency virus type 1 subtype C (HIV-1C) has a natural deletion of a YPxL motif in its Gag-p6 late domain. This domain mediates the binding of Gag to host cell protein ALIX and subsequently facilitates viral budding. In a subset of HIV-1C-infected individuals, the tetrapeptide insertion PYxE has been identified at the deleted YPxL motif site. Here, we report the consequences of PYxE insertion on the interaction with ALIX and the relevance regarding replication fitness and drug sensitivity. In our three HIV-1C cohorts, PYKE and PYQE were most prevalent among PYxE variants. Through in silico predictions and in vitro experiments, we showed that HIV-1C Gag has an increased binding to ALIX when the PYxE motif is present. To go more into the clinical relevance of the PYxE insertion, we obtained patient-derived gag-pol sequences from HIV-1CPYxEi viruses and inserted them in a reference HIV-1 sequence. Viral growth was increased, and the sensitivity to the protease inhibitor (PI) lopinavir (LPV) and nucleoside reverse transcriptase inhibitor tenofovir alafenamide (TAF) was decreased for some of the HIV-1C PYxE variants compared to that of wild-type variants. Our data suggest that PYxE insertion in Gag restores the ability of Gag to bind ALIX and correlates with enhanced viral fitness in the absence or presence of LPV and TAF. The high prevalence and increased replication fitness of the HIV-1C virus with PYxE insertion indicates the clinical importance of these viral variants. IMPORTANCE Genomic differences within HIV-1 subtypes is associated with various degrees of viral spread, disease progression, and clinical outcome. Viral budding is essential in the HIV-1 life cycle and mainly mediated through the interaction of Gag with host proteins. Two motifs within Gag-p6 mediate binding of host cell proteins and facilitate budding. HIV-1C has a natural deletion of one of these two motifs, resulting in an inability to bind to host cell protein ALIX. Previously, we have identified a tetrapeptide (PYxE) insertion at this deleted motif site in a subset of HIV-1C patients. Here, we report the incidence of PYxE insertions in three different HIV-1C cohorts, and the insertion restores the binding of Gag to ALIX. It also increases viral growth even in the presence of the antiretroviral drugs lopinavir and tenofovir alafenamide. Hence, PYxE insertion in HIV-1C might be biologically relevant for viruses and clinically significant among patients.

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HIV-1 subtype C with PYxE insertion has enhanced binding of Gag-p6 to host cell protein ALIX and increased replication fitness

Cited by 3 publications

References 40 publications

Cytotoxic Lymphocytes Target HIV-1 Gag Through Granzyme M-Mediated Cleavage

Cytotoxic Lymphocytes Target HIV-1 Gag Through Granzyme M-Mediated Cleavage

Cytotoxic lymphocytes target HIV-1 Gag through granzyme M-mediated cleavage

HIV-1 Subtype C with PYxE Insertion Has Enhanced Binding of Gag-p6 to Host Cell Protein ALIX and Increased Replication Fitness

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