Characterization of T-Cell Responses to Conserved Regions of the HIV-1 Proteome in BALB/c Mice

Ondondo, Beatrice; Abdul-Jawad, Sultan; Bridgeman, Anne; Hanke, Tomáš

doi:10.1128/cvi.00587-14

Cited by 19 publications

(19 citation statements)

References 42 publications

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“…The PBMCs were thawed, and an equal volume of RPMI supplemented with 10% FCS (RPMI10) plus 50 U/ml Benzonase nuclease (Novagen) warmed to 37°C was added dropwise. Cells were expanded by using pools 1 to 6 of HIVconsv-derived 15-mer peptides overlapping by 11 amino acids (aa) ( 22 ) for 10 days, rested, and tested by a gamma interferon (IFN-γ) enzyme-linked immunosorbent spot (ELISPOT) assay as described previously ( 27 ). Thus, ELISPOT plates (catalog number S5EJ044I10; Merck Millipore) prewetted for 1 min with 15 μl of 35% ethanol were coated overnight at +4°C with anti-IFN-γ antibody (10 μg/ml in PBS) (clone 1-D1K; Mabtech).…”

Section: Methodsmentioning

confidence: 99%

Early Kinetics of the HLA Class I-Associated Peptidome of MVA.HIVconsv-Infected Cells

Ternette

Block

Sánchez-Bernabéu

et al. 2015

J Virol

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Cytotoxic T cells substantially contribute to the control of intracellular pathogens such as human immunodeficiency virus type 1 (HIV-1). Here, we evaluated the immunopeptidome of Jurkat cells infected with the vaccine candidate MVA.HIVconsv, which delivers HIV-1 conserved antigenic regions by using modified vaccinia virus Ankara (MVA). We employed liquid chromatography-tandem mass spectrometry (LC-MS/MS) to identify 6,358 unique peptides associated with the class I human leukocyte antigen (HLA), of which 98 peptides were derived from the MVA vector and 7 were derived from the HIVconsv immunogen. Human vaccine recipients responded to the peptide sequences identified by LC-MS/MS. Peptides derived from the conserved HIV-1 regions were readily detected as early as 1.5 h after MVA.HIVconsv infection. Four of the seven conserved peptides were monitored between 0 and 3.5 h of infection by using quantitative mass spectrometry (Q-MS), and their abundance in HLA class I associations reflected levels of the whole HIVconsv protein in the cell. While immunopeptides delivered by the incoming MVA vector proteins could be detected, all early HIVconsv-derived immunopeptides were likely synthesized de novo. MVA.HIVconsv infection generally altered the composition of HLA class I-associated human (self) peptides, but these changes corresponded only partially to changes in the whole cell host protein abundance.IMPORTANCE The vast changes in cellular antigen presentation after infection of cells with a vectored vaccine, as shown here for MVA.HIVconsv, highlight the complexity of factors that need to be considered for efficient antigen delivery and presentation. Identification and quantitation of HLA class I-associated peptides by Q-MS will not only find broad application in T-cell epitope discovery but also inform vaccine design and allow evaluation of efficient epitope presentation using different delivery strategies.

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Section: Methodsmentioning

confidence: 99%

Early Kinetics of the HLA Class I-Associated Peptidome of MVA.HIVconsv-Infected Cells

Ternette

Block

Sánchez-Bernabéu

et al. 2015

J Virol

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“…Cytokine production by splenocytes from immunized mice was assessed by intracellular cytokine staining as described previously. 52 Briefly, splenocytes were stimulated individual peptides for 90 minutes at 37 °C, and then for further 5 hours in the presence of brefeldin A (Golgiplug, BD Biosciences) to prevent cytokine secretion. Cells were surface stained with anti-CD4-Pacific blue, anti-CD8-PE-Texas red (both eBioscience) antibodies and LIVE/DEAD fixable aqua dead cell stain (Invitrogen), and then permeabilized and incubated with various combinations of anti-IL-2-fluoroscein isothiocyanate, anti-IL-4-PE, anti-TNF-α-PE and anti-IFN-γ-APC monoclonal antibodies (Biolegend).…”

Section: Peptidesmentioning

confidence: 99%

“…Killing assay was performed as described previously. 52 Equal numbers of naive HHD splenocytes were differentially labeled with either 800 or 32 nmol/l of CFSE according to the manufacturer's specifications. Splenocytes from immunized mice were prepared as described above, mixed with the differentially CFSE-labeled target cells at an effectorto-target (ET) ratio of 10:1 or 5:1 and incubated overnight at 37 °C.…”

Section: Peptidesmentioning

confidence: 99%

Increased Valency of Conserved-mosaic Vaccines Enhances the Breadth and Depth of Epitope Recognition

et al. 2016

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The biggest roadblock in development of effective vaccines against human immunodeficiency virus type 1 (HIV-1) is the virus genetic diversity. For T-cell vaccine, this can be tackled by focusing the vaccine-elicited T-cells on the highly functionally conserved regions of HIV-1 proteins, mutations in which typically cause a replicative fitness loss, and by computing multivalent mosaic proteins, which maximize the coverage of potential 9-mer T-cell epitopes of the input viral sequences. Our first conserved region vaccines HIVconsv employed clade alternating consensus sequences and showed promise in the initial clinical trials in terms of magnitude and breadth of elicited CD8(+) T-cells. Here, monitoring T-cells restricted by HLA-A*02:01 in transgenic mice, we assessed whether or not the tHIVconsv design (HIVconsv with a tissue plasminogen activator leader sequence) benefits from combining with a complementing conserved mosaic immunogen tHIVcmo, and compared the bivalent immunization to that with trivalent conserved mosaic vaccines. A hierarchy of tHIVconsv ≤ tHIVconsv+tHIVcmo < tCmo1+tCmo2+tCmo3 vaccinations for induction of CD8(+) T-cell responses was observed in terms of recognition of tested peptide variants. Thus, our HLA-A*02:01-restricted epitope data concur with previously published mouse and macaque observations and suggest that even conserved region vaccines benefit from oligovalent mosaic design.

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“…Conserved sequences and immune responses have been characterized in animals [147,148], conferring partial protection against SIVmac251 in macaques [149]. In humans, a combination of DNA, ChAd63 and MVA vectors was found safe [150] and immunogenic, inducing high levels of effector T cells that recognized virus-infected autologous CD4+ cells.…”

Section: Hiv-1 Conserved Sequencesmentioning

confidence: 99%

Prospects for a Globally Effective HIV-1 Vaccine

Excler

Robb

Kim

2015

American Journal of Preventive Medicine

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A globally effective vaccine strategy must cope with the broad genetic diversity of HIV and contend with multiple transmission modalities. Understanding correlates of protection and the role of diversity in limiting protective vaccines with those correlates is key. RV144 was the first HIV-1 vaccine trial to demonstrate efficacy against HIV-1 infection. A correlates analysis comparing vaccine-induced immune responses in vaccinated-infected and vaccinated-uninfected volunteers suggested that IgG specific for the V1V2 region of gp120 was associated with reduced risk of HIV-1 infection and that plasma Env IgA was directly correlated with infection risk. RV144 and recent non-human primate (NHP) challenge studies suggest that Env is essential and perhaps sufficient to induce protective antibody responses against mucosally acquired HIV-1. Whether RV144 immune correlates can apply to different HIV vaccines, to populations with different modes and intensity of transmission, or to divergent HIV-1 subtypes remains unknown. Newer prime-boost mosaic and conserved sequence immunization strategies aiming at inducing immune responses of greater breadth and depth as well as the development of immunogens inducing broadly neutralizing antibodies should be actively pursued. Efficacy trials are now planned in heterosexual populations in southern Africa and men who have sex with men in Thailand. Although NHP challenge studies may guide vaccine development, human efficacy trials remain key to answer the critical questions leading to the development of a global HIV-1 vaccine for licensure.

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Characterization of T-Cell Responses to Conserved Regions of the HIV-1 Proteome in BALB/c Mice

Cited by 19 publications

References 42 publications

Early Kinetics of the HLA Class I-Associated Peptidome of MVA.HIVconsv-Infected Cells

Early Kinetics of the HLA Class I-Associated Peptidome of MVA.HIVconsv-Infected Cells

Increased Valency of Conserved-mosaic Vaccines Enhances the Breadth and Depth of Epitope Recognition

Prospects for a Globally Effective HIV-1 Vaccine

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