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A virologist’s guide to hide and seek : evasion of innate immunity by primate lentiviruses

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posted on 2024-09-02, 22:47 authored by Susanna Bächle

HIV is the cause of a chronic, incurable infection in 37 million people worldwide in 2014. This thesis investigates how the immune system detects HIV and how in turn HIV avoids detection by the immune system. The understanding of the viral evasion mechanisms that prevent immune detection (“Hide and Seek”) is important to successfully develop future vaccines and cure strategies for HIV.

Primate lentiviruses belong to the retrovirus family and include the human immunodeficiency viruses (HIV-1 and HIV-2) and simian immunodeficiency viruses (SIV). HIV infects cells of the immune system, including subsets of T cells and dendritic cells (DC). Upon cell entry, the detection of the virus by cellular pattern recognition receptors triggers an intracellular cascade of innate antiviral defense mechanisms. In DCs, these mechanisms include the secretion of interferon α and the induction of cellular restriction factors, among these members of the APOBEC3 family that inhibit viral replication. As demonstrated in Paper III, low doses of interferon α protected DCs from HIV-1 infection and limited viral spread from DCs to T cells by inducing an increase in APOBEC3G, F and A expression.

DCs are professional antigen presenting cells that present antigen to cells of the innate and adaptive immune system. Invariant natural killer T cells (iNKT) cells are innate T cells that recognize endogenous and exogenous lipid antigens presented by CD1d. Activated iNKT cells regulate the immune response by producing cytokines that recruit and activate innate and adaptive immune cells. Previous studies have shown that the HIV-1 accessory proteins Vpu and Nef interfere with CD1d cell surface expression in infected DCs, thus inhibiting the effective activation of iNKT cells. The results of Paper II demonstrated that infected DCs respond to HIV-1 infection by increasing CD1d surface levels and enhanced presentation of the endogenous lipid GlcCer. This enabled iNKT cell activation by HIV-infected DCs. However, HIV-1 counteracts iNKT cell activation by reducing CD1d cell surface expression using the HIV-1 proteins Nef and Vpu. In Paper I, efforts to elucidate the mechanism of CD1d antagonism by Vpu identified a highly conserved C-terminal APW motif in HIV-1 group M subtype B Vpu proteins that was necessary for CD1d downregulation. Moreover, we identified this immune evasion mechanism to be a conserved function of diverse HIV-1 and related SIV Vpus. These findings emphasize the role of CD1d-mediated immunity in the antiviral defense against HIV-1 and support the need for further studies investigating the therapeutic potential of Vpu inhibition in the future.

Previous studies found that innate cellular immune responses are altered in chronic HIV-1 infection. Our results in Paper IV from an occupational cohort in Guinea-Bissau suggest that this is a general phenomenon of chronic HIV infection as NK and iNKT cells were partly lost and the remaining populations displayed elevated activation levels in chronic HIV-1, HIV-2, and dual infections.

List of scientific papers

I. Bächle SM, Sauter D, Sibitz S, Sandberg JK, Kirchhoff F, Moll M. 2015. Involvement of a C-terminal motif in the interference of primate lentiviral Vpu proteins with CD1d-mediated antigen presentation. Scientific Reports.
https://doi.org/10.1038/srep09675

II. Paquin-Proulx D, Gibbs A, Bächle SM, Checa A, Introini A, Leeansyah E, Wheelock CE, Nixon DF, Broliden K, Tjernlund A, Moll M, Sandberg JK. Innate iNKT cell recognition of HIV-infected dendritic cells via induced expression of endogenous glycolipid antigen. [Manuscript]

III. Mohanram V, Sköld AE, Bächle SM, Pathak SK, Spetz AL. 2013. IFN-α induces APOBEC3G, F, and A in immature dendritic cells and limits HIV-1 spread to CD4+ T cells. Journal of Immunology.
https://doi.org/10.4049/jimmunol.1201184

IV. Bächle SM, Malone DFG, Buggert M, Karlsson AC, Isberg PE, Biague A, Norrgren H, Medstrand P, the SWEGUB CORE group, Moll M, Sandberg JK, Jansson M. Elevated levels of iNKT and NK cell activation correlate with disease progression in HIV-1 and HIV-2 infections. [Manuscript]

History

Defence date

2015-09-21

Department

  • Department of Medicine, Huddinge

Publisher/Institution

Karolinska Institutet

Main supervisor

Moll, Markus

Publication year

2015

Thesis type

  • Doctoral thesis

ISBN

978-91-7676-030-7

Number of supporting papers

4

Language

  • eng

Original publication date

2015-08-28

Author name in thesis

Bächle, Susanna M

Original department name

Department of Medicine, Huddinge

Place of publication

Stockholm

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