Journal
FRONTIERS IN IMMUNOLOGY
Volume 12, Issue -, Pages -Publisher
FRONTIERS MEDIA SA
DOI: 10.3389/fimmu.2021.669347
Keywords
cytotoxic lymphocyte; granzyme M; Gag (HIV-1); HIV-1; immune control
Categories
Funding
- Swedish Research Council [2016-01675, 2017-05848]
- CARE [825673]
- Stockholm County Council [ALF 20190451, CIMED 20200645]
- Swedish Research Council Establishment Grant [2017-01330]
- Swedish Physicians Against AIDS Research Foundation [Fob2017-0005]
- Stiftelsen Tornspiran
- KI Research Foundation [2018-01640]
- Swedish Research Council [2017-01330, 2017-05848] Funding Source: Swedish Research Council
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Untreated HIV-1 infection leads to a decrease in CD4(+) T cell lymphocytes, susceptibility to opportunistic infections, and ultimately death. This study found that cytotoxic lymphocytes can target the HIV-1 Gag protein through granzyme cleavage to potentially control HIV-1 infection.
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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