HIVconsv Vaccines and Romidepsin in Early-Treated HIV-1-Infected Individuals: Safety, Immunogenicity and Effect on the Viral Reservoir (Study BCN02)

Mothe, Beatriz; Rosás-Umbert, Míriam; Coll, Pep; Manzardo, Christian; Puertas, María C.; Morón-López, Sara; Llano, Anuska; Miranda, Cristina; Cedeño, Samandhy; López, Miriam; Alarcón-Soto, Yovaninna; Melis, Guadalupe Gómez; Langohr, Klaus; Barriocanal, Ana María; Toro, Jessica; Ruíz, Irene; Rovira, Carlos; Carrillo, Antonio; Meulbroek, Michael; Crook, Alison; Wee, Edmund G.; Miró, José M.; Clotet, Bonaventura; Valle, Marta; Martínez-Picado, Javier; Hanke, Tomáš; Berthou, Christian; Moltó, José

doi:10.3389/fimmu.2020.00823

Cited by 68 publications

(86 citation statements)

References 58 publications

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“…This was not the case following HIVconsv vaccination, which induced prominent Pol epitope responses directly proportional to the relative length of the Pol segment in the HIVconsv sequence (Table 3). These results would support the ability of a potent vector delivery to (re)focus immune responses including CD4 + T cells toward regions that are generally subdominant in natural HIV-1 infection [59,60]. A different study reported over half of tested variant peptides not being recognized by CD4 + T cells [51], emphasizing even for the more promiscuous HLA class II molecules peptide selectivity and the importance of focusing on and matching vaccine responses to less variable regions of the HIV-1 proteome.…”

Section: Discussionmentioning

confidence: 71%

Novel Nested Peptide Epitopes Recognized by CD4+ T Cells Induced by HIV-1 Conserved-Region Vaccines

et al. 2020

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CD4+ T-cell responses play an important role in the immune control of the human immunodeficiency virus type 1 (HIV-1) infection and as such should be efficiently induced by vaccination. It follows that definition of HIV-1-derived peptides recognized by CD4+ T cells in association with HLA class II molecules will guide vaccine development. Here, we have characterized the fine specificity of CD4+ T cells elicited in human recipients of a candidate vaccine delivering conserved regions of HIV-1 proteins designated HIVconsv. The majority of these 19 most immunogenic regions contained novel epitopes, that is, epitopes not listed in the Los Alamos National Laboratory HIV Sequence Database, which were able in vitro to stimulate vaccinees’ CD4+ T cells to proliferate and produce interferon-γ and tumor necrosis factor-α. Accumulation of HLA class II epitopes will eventually accelerate development of HIV-1 prophylactic and therapeutic vaccines.

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Section: Discussionmentioning

confidence: 71%

Novel Nested Peptide Epitopes Recognized by CD4+ T Cells Induced by HIV-1 Conserved-Region Vaccines

et al. 2020

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“…The GRIN immunogen was a fusion of full-length Gag, Reverse Transcriptase (RT), Integrase and Nef, and was delivered by replication-deficient human adenovirus serotype 35 (Ad35-GRIN or A) [ 66 , 67 ]. Ad35-GRIN substituted for the simian adenovirus serotype 63-vectored HIVconsv vaccine used in previous trials [ 50 , 56 , 57 , 58 , 59 ], to which we lost freedom to operate following GlaxoSmithKline acquisition of the ChAdV63 vaccine vector. GRIN had an extensive sequence match to HIVconsv as GRIN covered almost 80% of all HIVconsv ( Figure 1 ) [ 60 ].…”

Section: Resultsmentioning

confidence: 99%

“…In contrast, our working hypothesis postulates that focusing vaccine-elicited T cells on the functionally conserved regions of HIV-1, which are common to most global variants and are hard to mutate, will be effective in slowing and controlling HIV-1 infection [ 41 , 42 , 43 , 50 , 51 , 52 , 53 , 54 , 55 ]. These regions contain epitopes typically subdominant in natural HIV-1 infection, but are capable of inducting robust T-cell responses when delivered by a potent vaccination regimen [ 50 , 56 , 57 , 58 , 59 , 60 ]. Such vaccine-elicited responses thus represent a rich source of previously undescribed, potentially important epitopes [ 61 , 62 , 63 ].…”

Section: Introductionmentioning

confidence: 99%

Specificity of CD8+ T-Cell Responses Following Vaccination with Conserved Regions of HIV-1 in Nairobi, Kenya

et al. 2020

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Sub-Saharan Africa carries the biggest burden of the human immunodeficiency virus type 1 (HIV-1)/AIDS epidemic and is in an urgent need of an effective vaccine. CD8+ T cells are an important component of the host immune response to HIV-1 and may need to be harnessed if a vaccine is to be effective. CD8+ T cells recognize human leukocyte antigen (HLA)-associated viral epitopes and the HLA alleles vary significantly among different ethnic groups. It follows that definition of HIV-1-derived peptides recognized by CD8+ T cells in the geographically relevant regions will critically guide vaccine development. Here, we study fine details of CD8+ T-cell responses elicited in HIV-1/2-uninfected individuals in Nairobi, Kenya, who received a candidate vaccine delivering conserved regions of HIV-1 proteins called HIVconsv. Using 10-day cell lines established by in vitro peptide restimulation of cryopreserved PBMC and stably HLA-transfected 721.221/C1R cell lines, we confirm experimentally many already defined epitopes, for a number of epitopes we define the restricting HLA molecule(s) and describe four novel HLA-epitope pairs. We also identify specific dominance patterns, a promiscuous T-cell epitope and a rescue of suboptimal T-cell epitope induction in vivo by its functional variant, which all together inform vaccine design.

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“…Total DNA is the quantification of all forms of HIV-DNA, integrated and unintegrated, coding for both competent and defective viruses reflecting the global size of the reservoir giving an overview of its distribution in the body at all stages of the disease [ 66 ]. Several studies testing different therapeutic based-vaccine strategies (alone, boosted or combined) [ 33 , 37 , 44 , 45 , 50 , 65 , 67 ] ( Table 4 ), have measured total DNA as a reservoir biomarker and found different results when assessing the effect on pVL during ATI. Some of these studies, one conducted in patients that started ART during acute infection [ 45 ], have described a correlation between a smaller size of baseline CA-DNA and longer time to resume ART after ATI [ 33 , 50 ], but some others found no relation [ 37 , 44 , 67 ].…”

Section: Surrogate Markers Of Viral Response During Atimentioning

confidence: 99%

“…Several studies testing different therapeutic based-vaccine strategies (alone, boosted or combined) [ 33 , 37 , 44 , 45 , 50 , 65 , 67 ] ( Table 4 ), have measured total DNA as a reservoir biomarker and found different results when assessing the effect on pVL during ATI. Some of these studies, one conducted in patients that started ART during acute infection [ 45 ], have described a correlation between a smaller size of baseline CA-DNA and longer time to resume ART after ATI [ 33 , 50 ], but some others found no relation [ 37 , 44 , 67 ]. Neither of these studies found any significant effect on CA-DNA of any of the studied products, although a study evaluating a DC-based vaccine found that the magnitude of T cell responses measured by IFNγ ELISPOT during the vaccination period was an independent predictor of total DNA during ATI and also found a correlation between total DNA levels and pVL set point during ATI [ 44 ].…”

Section: Surrogate Markers Of Viral Response During Atimentioning

confidence: 99%

Antiretroviral Therapy Interruption (ATI) in HIV-1 Infected Patients Participating in Therapeutic Vaccine Trials: Surrogate Markers of Virological Response

et al. 2020

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A functional Human immunodeficiency Virus (HIV) cure has been proposed as an alternative to antiretroviral treatment for life, and therapeutic vaccines represent one of the most promising approaches. The goal of therapeutic vaccination is to augment virus-specific immune responses that have an impact on HIV viral load dynamics. To date, the agreed feature to evaluate the effects of these therapeutic interventions is analytical antiretroviral treatment interruption (ATI), at least until we find a reliable biomarker that can predict viral control. Different host, immunologic, and virologic markers have been proposed as predictors of viral control during ATI after therapeutic interventions. This review describes the relevance of ATI and the different surrogate markers of virological control assessed in HIV therapeutic vaccine clinical trials.

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HIVconsv Vaccines and Romidepsin in Early-Treated HIV-1-Infected Individuals: Safety, Immunogenicity and Effect on the Viral Reservoir (Study BCN02)

Cited by 68 publications

References 58 publications

Novel Nested Peptide Epitopes Recognized by CD4+ T Cells Induced by HIV-1 Conserved-Region Vaccines

Novel Nested Peptide Epitopes Recognized by CD4+ T Cells Induced by HIV-1 Conserved-Region Vaccines

Specificity of CD8+ T-Cell Responses Following Vaccination with Conserved Regions of HIV-1 in Nairobi, Kenya

Antiretroviral Therapy Interruption (ATI) in HIV-1 Infected Patients Participating in Therapeutic Vaccine Trials: Surrogate Markers of Virological Response

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