Variable Processing and Cross-presentation of HIV by Dendritic Cells and Macrophages Shapes CTL Immunodominance and Immune Escape

Dinter, Jens; Duong, Ellen; Lai, Nicole Y.; Berberich, Matthew J.; Kourjian, Georgio; Bracho-Sanchez, Edith; Chu, Duong; Su, Hang; Zhang, Shao Chong; Gall, Sylvie Le

doi:10.1371/journal.ppat.1004725

Cited by 30 publications

(48 citation statements)

References 75 publications

(114 reference statements)

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“…While some cleavage sites were shared among all three cell types, some, such as the cleavage at P position 9 in 293T, appeared uniquely in one cell subset and increased in abundance over time. The cell type-specific degradation patterns are in accordance with our previous findings (19,28,34). While some peptides such as AQ14 (ASLRSLFGSDPSSQ) were produced in extracts from all three cell types and displayed by all of them, others such as RQ11 (RSLFGSDPSSQ) were produced by all subsets but displayed by only one or two cell types, showing that the presentation of these peptides is limited not by cell type-specific production but rather by the HLAs of the cells.…”

Section: Peptides Eluted From Live Cells Identify Additional Hiv-specsupporting

confidence: 90%

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Analysis of Major Histocompatibility Complex-Bound HIV Peptides Identified from Various Cell Types Reveals Common Nested Peptides and Novel T Cell Responses

Ručević

Kourjian

Boucau

et al. 2016

J Virol

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H IV-specific T cells play an important role in the containment of infection as evidenced by the concurrent drop of viral load and the appearance of HIV-specific CD8 T cells in acute infection, T cell-driven immune pressure leading to predictable HLA-restricted HIV mutations, and the association between specific HLAs and epitopes or immune responses to specific proteins and spontaneous control of HIV. However, the lack of clear correlates of immune protection hampers efficient vaccine design (1).Screening and functional studies of T cells from HIV-infected persons or vaccinees use high nonphysiological concentrations of long HIV peptides exogenously pulsed onto cells or soluble major histocompatibility complex (MHC)-peptide multimers presenting peptides of optimal size (2, 3). These approaches bypass all steps required for intracellular antigen processing and presentation of HIV peptides by MHC class I (MHC-I) molecules (4). Determination of the amounts and sequences of peptides presented by an infected cell remains largely elusive despite the role of the peptides in immune recognition.Direct mass spectrometry (MS)-based sequencing has become a preferred and yet difficult approach for the unbiased identification and characterization of peptides naturally presented by MHC-I molecules displayed by healthy and cancerous cells or in the context of pathogen infection. However, considering the relatively low number of MHC-peptide complexes per cell and the

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Section: Peptides Eluted From Live Cells Identify Additional Hiv-specsupporting

confidence: 90%

“…The degradation was stopped with 2.5 l of 100% formic acid, and peptide fragments were purified by the use of 5% trichloroacetic acid (TCA) precipitation. Degradation peptides generated in 2 to 3 independent degradation experiments were identified by in-house LC/MS-MS as previously described (20,21,28).…”

Section: Methodsmentioning

confidence: 99%

Analysis of Major Histocompatibility Complex-Bound HIV Peptides Identified from Various Cell Types Reveals Common Nested Peptides and Novel T Cell Responses

Ručević

Kourjian

Boucau

et al. 2016

J Virol

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“…The degradation was stopped with 2.5μL of 100% formic acid and peptide fragments were purified by 5% trichloroacetic acid precipitation. Degradation peptides were identified by in-house MS as previously described (8, 19). …”

Section: Methodsmentioning

confidence: 99%

“…Proteolytic activity measurement was performed as we previously described in (8, 19, 25). Briefly, 5x104 DCs, Møs or CD4T cells were pretreated with indicated PIs and omnicathepsin, cathepsin S, cathepsin D or cathepsin E activities were measured using Z-FR-AMC, Z-VVR-AMC, Ac-RGFFP-AMC or MOCAc-GSPAFLAK-Dnp-R specific fluorogenic substrates respectively.…”

Section: Methodsmentioning

confidence: 99%

“…Upon phagocytosis, phagosomes fuse with early and late endosomes and with lysosomes, thus acquiring progressively both the acidification machinery (mainly the V-ATPase complex) and lysosomal proteases (18). Acidification results in the activation of cathepsins with optimal proteolytic activities between pH 4-6 (18, 19). The activation and recruitment of NADPH oxidase 2 (NOX2) at the phagosomal membrane generates reactive oxygen species (ROS), increasing pH and limiting cathepsin activities and antigen degradation in DCs (20, 21).…”

Section: Introductionmentioning

confidence: 99%

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HIV Protease Inhibitor–Induced Cathepsin Modulation Alters Antigen Processing and Cross-Presentation

Kourjian

Ručević

Berberich

et al. 2016

The Journal of Immunology

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Immune recognition by T cells relies on the presentation of pathogen-derived peptides by infected cells but the persistence of chronic infections calls for new approaches to modulate immune recognition. Antigen cross-presentation, the process by which pathogen antigens are internalized, degraded and presented by MHC-I is crucial to prime CD8 T cell responses. The original degradation of antigens is performed by pH-dependent endolysosomal cathepsins. Here we show that HIV protease inhibitors (PIs) prescribed to HIV-infected persons variably modulate cathepsin activities in human antigen presenting cells (APCs), dendritic cells and macrophages, and CD4 T cells, three cell subsets infected by HIV. Two HIV PIs acted in two complementary ways on cathepsin hydrolytic activities: directly on cathepsins and indirectly on their regulators by inhibiting Akt kinase activities, reducing NADPH oxidase 2 (NOX2) activation, lowering phagolysosomal ROS production and pH, which altogether led to enhanced cathepsin activities. HIV PIs modified endolysosomal degradation and epitope production of proteins from HIV and other pathogens in a sequence-dependent manner. They altered cross-presentation of antigens by dendritic cells to epitope-specific T cells and T cell-mediated killing. HIV PI-induced modulation of antigen processing partly changed the self MHC-peptidome displayed by primary human cells. This first identification of prescription drugs modifying the regulation of cathepsin activities and the MHC-peptidome may provide an alternate therapeutic approach to modulate immune recognition in immune disease beyond HIV.

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Investigation of Immunostimulatory Effects of IFN‐γ Cytokine and CD40 Ligand Costimulatory Molecule for Development of HIV‐1 Therapeutic Vaccine Candidate

Heidarnejad,

Bolhassani,

Ajdary

et al. 2023

Advanced Biology

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The most crucial disadvantage of DNA‐based vaccines is their low immunogenicity; therefore, finding an effectual adjuvant is essential for their development. Herein, immunostimulatory effects of IFNγ cytokine and a CD40 ligand (CD40L) costimulatory molecule are evaluated as combined with an antigen, and also linked to an antigen in mice. For this purpose, after preparation of the HIV‐1 Nef, IFNγ, and CD40L DNA constructs, and also their recombinant protein in an Escherichia coli expression system, nine groups of female BALB/c mice are immunized with different regimens of DNA constructs. About 3 weeks and also 3 months after the last injection, humoral and cellular immune responses are assessed in mice sera and splenocytes. Additionally, mice splenocytes are exposed to single‐cycle replicable (SCR) HIV‐1 virions for evaluating their potency in the secretion of cytokines in vitro. The data indicate that the linkage of IFNγ and CD40L to Nef antigen can significantly induce the Th‐1 pathway and activate cytotoxic T lymphocytes compared to other regimens. Moreover, groups receiving the IFNγ‐Nef and CD40L‐Nef fusion DNA constructs show higher secretion of IFNγ and TNF‐α from virion‐infected lymphocytes than other groups. Therefore, the IFNγ‐Nef and CD40L‐Nef fusion DNA constructs are suggested to be a potential option for development of an efficient HIV‐1 vaccine.

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Variable Processing and Cross-presentation of HIV by Dendritic Cells and Macrophages Shapes CTL Immunodominance and Immune Escape

Cited by 30 publications

References 75 publications

Analysis of Major Histocompatibility Complex-Bound HIV Peptides Identified from Various Cell Types Reveals Common Nested Peptides and Novel T Cell Responses

Analysis of Major Histocompatibility Complex-Bound HIV Peptides Identified from Various Cell Types Reveals Common Nested Peptides and Novel T Cell Responses

HIV Protease Inhibitor–Induced Cathepsin Modulation Alters Antigen Processing and Cross-Presentation

Investigation of Immunostimulatory Effects of IFN‐γ Cytokine and CD40 Ligand Costimulatory Molecule for Development of HIV‐1 Therapeutic Vaccine Candidate

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