Gene Expression Signatures Associated With Immune and Virological Responses to Therapeutic Vaccination With Dendritic Cells in HIV-Infected Individuals

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2019 May 21

PMID 31105698

Citations 7

Authors

Rodolphe Thiebaut

Boris P Hejblum

Hakim Hocini

Henri Bonnabau

Jason Skinner

Monica Montes

Christine Lacabaratz

Laura Richert

Karolina Palucka

Jacques Banchereau

Yves Levy

Affiliations

Soon will be listed here.

Abstract

The goal of HIV therapeutic vaccination is to induce HIV-specific immune response able to control HIV replication. We previously reported that vaccination with generated Dendritic Cells (DC) loaded with HIV-lipopeptides in HIV-infected patients ( = 19) on antiretroviral therapy (ART) was well-tolerated and immunogenic. Vaccine-elicited HIV-specific T cell responses were associated with improved control of viral replication following antiretroviral interruption (ATI from w24 to w48). We show an inverse relationship between HIV-specific responses (production of IL-2, IL-13, IL-21, IFN-g, CD4 polyfunctionality, i.e., production of at least two cytokines) and the peak of viral load during ATI. Here we have performed an integrative systems vaccinology analysis including: (i) post vaccination (w16) immune responses assessed by cytometry, cytokine secretion, and Interferon-γ ELISPOT assays; (ii) whole blood and cellular gene expression measured during vaccination; and (iii) viral parameters following ATI, with the objective to disentangle the relationships between these markers and to identify vaccine signatures. During vaccination, 69 gene expression modules out of 260 varied significantly including (by order of significance) modules related to inflammation (Chaussabel Modules M3.2, M4.13, M4.6, M5.7, M7.1, M4.2), plasma cells (M4.11) and T cells (M4.1, 4.15). Cellular immune responses were positively correlated to genes belonging to T cell functional modules (M4.1, M4.15) at w16 and negatively correlated to genes belonging to inflammation modules (M7.1, M5.7, M3.2, M4.13, M4.2). More specifically, we show that prolonged increased abundance of inflammatory gene pathways related to toll-like receptor signaling (especially TLR4) are associated with both lower vaccine immune responses and control of viral replication post ATI. Further comparison of DC vaccine gene signatures with previously reported non-HIV vaccine signatures, such as flu and pneumococcal vaccines, revealed common pathways across vaccines. Overall, these results show that too long duration and too high intensity of vaccine inflammatory responses hamper the magnitude of effector responses.

Citing Articles

Differential immune transcriptomic profiles between vaccinated and resolved HCV reinfected subjects.

Mazouz S, Salinas E, Bedard N, Filali A, Khedr O, Swadling L PLoS Pathog. 2022; 18(11):e1010968.

PMID: 36378682 PMC: 9707775. DOI: 10.1371/journal.ppat.1010968.

Association of Transcriptomic Signatures of Inflammatory Response with Viral Control after Dendritic Cell-Based Therapeutic Vaccination in HIV-1 Infected Individuals.

Feher C, Pastor-Lbanez R, Leal L, Plana M, Arnedo M, van den Ham H Vaccines (Basel). 2021; 9(7).

PMID: 34358215 PMC: 8310264. DOI: 10.3390/vaccines9070799.

Impact of Transcriptome and Gut Microbiome on the Response of HIV-1 Infected Individuals to a Dendritic Cell-Based HIV Therapeutic Vaccine.

Pastor-Ibanez R, Diez-Fuertes F, Sanchez-Palomino S, Alcami J, Plana M, Torrents D Vaccines (Basel). 2021; 9(7).

PMID: 34202658 PMC: 8310021. DOI: 10.3390/vaccines9070694.

A Randomized Placebo-Controlled Efficacy Study of a Prime Boost Therapeutic Vaccination Strategy in HIV-1-Infected Individuals: VRI02 ANRS 149 LIGHT Phase II Trial.

Levy Y, Lacabaratz C, Lhomme E, Wiedemann A, Bauduin C, Fenwick C J Virol. 2021; 95(9).

PMID: 33568510 PMC: 8104102. DOI: 10.1128/JVI.02165-20.

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

Leal L, Feher C, Richart V, Torres B, Garcia F Vaccines (Basel). 2020; 8(3).

PMID: 32764508 PMC: 7564579. DOI: 10.3390/vaccines8030442.

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