Phase II Trial of ART + Dual bNAbs vs. ART + Placebo During Primary HIV-1 Infection-impact on Post-ART Control

Phase 2RecruitingNCT05300035

ANRS, Emerging Infectious Diseases69 enrolled

Overview

RHIVIERA-02 trial is a placebo-controlled double-blinded two arm prospective phase II trial. This study will test the use of broadly neutralising antibodies (bNAbs) in participants, at primary HIV infection (PHI) and ART initiation.

The study proposes to test an intervention consisting of dual long-acting HIV-specific broadly neutralizing antibodies (3BNC117-LS \& 10-1074-LS ) + ART, at primary HIV-1 infection, and to compare it to ART only regarding HIV-1 replication. The study aims to enrol 69 participants in French (Ile-de-France) clinical centres. Participants will have been diagnosed with primary HIV-1 infection, will start ART during early phase of Primary HIV infection, and will interrupt ART 52 weeks later. Study duration will vary by participant, depending on the time of ART interruption and the time to viral rebound.

Study Type

INTERVENTIONAL

Allocation

RANDOMIZED

Purpose

TREATMENT

Masking

TRIPLE

Enrollment

Conditions

HIV/AIDS and Infections

Interventions

Recombinant human monoclonal antibody (bNAbs)DRUG

1. Initiation of combination ART (1 integrase inhibitor + 2 nucleoside analogue reverse transcriptase inhibitors) with additional dual intravenous infusions of bNAbs (3BNC117LS \& 10-1074LS) between Day 7 and Day 10. 2. Analytical treatment interruption (ATI), 52 weeks later, if good immunologic and virologic conditions. 3. During ATI, plasma HIV-1 RNA and CD4 monitoring, for a maximum of 48 weeks. 4. ART resumption, if participant encounters at least one ART resumption criteria.

PlaceboDRUG

1. Initiation of combination ART (1 integrase inhibitor + 2 nucleoside analogue reverse transcriptase inhibitors) with additional dual intravenous infusions of placebo (saline solution) between Day 7 and Day 10. 2. Analytical treatment interruption (ATI), 52 weeks later, if good immunologic and virologic conditions. 3. During ATI, plasma HIV-1 RNA and CD4 monitoring, for a maximum of 48 weeks. 4. ART resumption, if participant encounters at least one ART resumption criteria.

Eligibility

Sex: ALLMin age: 18 YearsMax age: 70 Years

Medical Language ↔ Plain English

Inclusion Criteria: * Confirmed primary HIV-1 infection diagnostic * Aged ≥18 to ≤70 years old at screening * Willing to use use an effective method of contraception from the inclusion until the end of the follow-up in the trial * Negative plasmatic beta human chorionic gonadotropin (β-HCG) pregnancy test, when applicable * Agree not to seek pregnancy including through alternative methods, such as artificial insemination or in vitro fertilization until after the last required protocol clinic visit, when applicable * Informed and written signed consent * Participant with regular health insurance * Willing to accept the trial constraints (travel for IMP administration and ART interruption) * Willing to be vaccinated against COVID-19 according to recommandations Exclusion Criteria: * Participation in any other clinical trial requiring additional blood sampling Participation in an observational study without additional blood sampling is permitted * Participants in whom condom use or PrEP use by the partner will be difficult or impossible * Pregnant or breastfeeding patient * Participants under guardianship or curatorship * Any condition or infection, including HCV, HBV, SARS-CoV-2 or known M. tuberculosis active infection History of ischemic heart disease (myocardial infarction, stable or unstable angina, stroke) * Current or past history of cancer, excluding squamous cell skin cancers * History or acute known inflammatory ophthalmic affection (uveitis, choroiditis, optic neuropathy) * Any medical condition that contraindicates ART interruption * Concomitant or previous conditions that preclude injection of monoclonal antibodies * History of systemic corticosteroids, immunosuppressive and anti-cancer medications within the last 6 months * History of severe reaction to a vaccine or drug infusion or history of severe allergic reactions * Individuals with any contraindication (including hypersensitivity reaction) to 3BNC117-LS and 10-1074-LS infusion * Prothrombin \< 50% * Creatinine clearance \< 60mL/mn (Cockroft) * ASAT or ALAT or bilirubine (total et conjugated) ≥ 10 times the upper limit of normal * Patient with an isolated HIV-2 viral strain * Planned absence that could affect participation in the trial (travel abroad, relocation, impending transfer...)

Locations (17)

Hôpial Avicenne - SMIT

Bobigny, France

RECRUITING

Hôpital Antoine Béclère

Clamart, France

Outcomes

Primary Outcomes

Proportion of participants with plasma HIV-1 RNA below 400 cp/mL 24 weeks following ATI (W24 ATI), in the confirmed absence of ART.

These participants will be considered as post-treatment controllers.

Time frame: at Week 24 of antiretroviral treatment interruption period (ATI)

Secondary Outcomes

Tolerance of bNAbs infusion : Number of clinical and biological adverse event (AE)

Number of clinical and biological AE during follow-up. Abnormal laboratory values will be identified as those outside values defined by the DAIDS scale

Time frame: from date of inclusion to the last follow-up visit date, up to 148 weeks

Tolerance of bNAbs infusion : Nature and Grade of clinical and biological AE

Grade of clinical and biological adverse during follow-up. The intensity of all AE (serious and non-serious) will be graded using the DAIDS AE Grading Table Corrected Version 2.1-July 2017

Time frame: from date of inclusion to the last follow-up visit date, up to 148 weeks

Tolerance of bNAbs infusion : Time of clinical and biological adverse event (AE)

Time frame: from date of inclusion to the last follow-up visit date, up to 148 weeks

Proportion of participants resuming ART within the first 24 weeks of ART interruption, according to the reason for resuming.

Time frame: at Week 24 of antiretroviral treatment interruption period (ATI)

Time to potential ART resumption for non-controllers.

Time frame: from Day 0 of antiretroviral treatment interruption period (ATI) to Day 0 of ART resumption date, assessed up to 48 weeks following ATI

Clinical and immulogical criteria during follow-up: Proportion of participants with clinical symptoms.

Central Contacts

Mathilde Ghislain, MSc

CONTACT

+331 45 59 52 29 mathilde.ghislain@inserm.fr

Nicolas Leturque, MSc

CONTACT

+331 45 59 51 93 nicolas.leturque@inserm.fr

Data from ClinicalTrials.gov

This platform is for informational purposes only and does not constitute medical advice. Always consult a qualified healthcare professional.

Hôpital Beaujon - Service de médecine interne

Clichy, France

RECRUITING

CHI Créteil - HdJ

Créteil, France

RECRUITING

Hôpital Raymond Poincaré - SMIT

Garches, France

RECRUITING

Hôpital Bicêtre - HdJ - Médecine interne

Le Kremlin-Bicêtre, France

RECRUITING

Hôpital Hôtel - Dieu

Paris, France

RECRUITING

Hôpital Hôtel Dieu - Service d'immunologie clinique

Paris, France

NOT_YET_RECRUITING

Hôpital Pitié-Salpêtrière - SMIT

Paris, France

RECRUITING

Hôpital Lariboisière - Service de médecine interne A

Paris, France

RECRUITING

...and 7 more locations

Time frame: during all ART period (from Day 0 to Week 52 ARV), during all ATI period (from Day 0 ATI to Day 0 ART Resumption) and during ART resumption period (from Day 0 to Week 24 ART Resumption)

Clinical and immulogical criteria during follow-up: Evolution of CD4, CD8 (levels and %) and CD4/CD8 ratio.

Time frame: during all ART period (from Day 0 to Week 52 ARV), during all ATI period (from Day 0 ATI to Day 0 ART Resumption) and during ART resumption period (from Day 0 to Week 24 ART Resumption)

Clinical and immulogical criteria during follow-up: Evolution of inflammation markers levels.

physiological parameters levels will be studied: IP10, TGFβ, IL-7, IL-10, IL-12, IL-15, IL-18, Citrulline, sCD14, sCD163, TNF-α

Time frame: biological parameters levels during all ART period (from Day 0 to Week 52 ARV), during all ATI period (from Day 0 ATI to Day 0 ART Resumption) and during ART resumption period (from Day 0 to Week 24 ART Resumption)

Immulogical criteria : Changes in the magnitude and quality of HIV-specific T cell responses and humoral responses.

physiological parameters levels will be studied: frequency and functionality of T cells responding to HIV peptides measured by intracellular cytokine staining, surface expression of activation and differentiation markers, HIV suppressive capacity upon co-culture with autologous infected cells

Time frame: physiological parameters levels during all ART period (from Day 0 to Week 52 ARV), during all ATI period (from Day 0 ATI to Day 0 ART Resumption) and during ART resumption period (from Day 0 to Week 24 ART Resumption)

Virological criteria during follow-up: Plasma HIV-1 RNA and HIV-1 DNA level and cell-associated HIV RNA transcripts changes.

Time frame: during all ART period (from Day 0 to Week 52 ARV), during all ATI period (from Day 0 ATI to Day 0 ART Resumption) and during ART resumption period (from Day 0 to Week 24 ART Resumption)

Virological criteria : Proportion of participant with plasma HIV-1 RNA < 50 cp/mL at 12- and 24-weeks following ART interruption.

Time frame: at Week 12 and Week 24 of antiretroviral treatment interruption period (ATI)

Virological criteria : Cumulative plasma viremia during ART interruption.

Time frame: from Day 0 of antiretroviral treatment interruption period (ATI) to Day 0 of ART resumption, assessed up to 48 weeks following ATI

Virological criteria : in case of ART resumption, time from date of ART interruption begining to date of first HIV-1 RNA ≥ 50 copies/mL

Time frame: from Day 0 of antiretroviral treatment interruption period (ATI) to Day 0 of ART resumption, assessed up to 48 weeks following ATI

Virological criteria : in case of ART resumption, proportion of participant with plasma HIV-1 RNA < 50 copies/mL within 24 weeks of ATI.

Time frame: from Day 0 of antiretroviral treatment interruption period (ATI) to Day 0 of ART resumption, assessed up to 48 weeks following ATI

Virological criteria : Evolution of total HIV-1 DNA and cell-associated HIV-1 RNA by US q-PCR and predictive value on post- ART interruption evolution.

Time frame: during all ART period (from Day 0 to Week 52 ARV), during all ATI period (from Day 0 ATI to Day 0 ART Resumption) and during ART resumption period (from Day 0 to Week 24 ART Resumption)

Virological criteria : Evolution of detection proportion and level of cell-associated HIV-1 RNA.

Time frame: during all ART period (from Day 0 to Week 52 ARV), during all ATI period (from Day 0 ATI to Day 0 ART Resumption) and during ART resumption period (from Day 0 to Week 24 ART Resumption)

Virological criteria : Qualitative and quantitative changes in the persistent viral reservoir.

physiological parameters levels will be studied: total cell associated HIV-DNA, integrated HIV-DNA, proportion of replication competent vs defective proviruses

Dosages of bNAbs performed during follow-up.

Time frame: during ART follow-up (Week 1,Week 12, Week 24, Week 36), and antiretroviral treatment interruption period (Day 0, Week 12, Week 24)

Criteria related to the risk of HIV-1 transmission : Proportion of participants reporting to use condoms during sexual intercourses

Time frame: from date of inclusion to the last follow-up visit date, up to 148 weeks

Criteria related to the risk of HIV-1 transmission : Proportion of participants reporting to have proposed PrEP at their partners.

Time frame: from date of inclusion to the last follow-up visit date, up to 148 weeks

Social sciences criteria : Proportion of patients satisfied with their participation and the associated factors

Time frame: from date of inclusion to the last follow-up visit date, up to 148 weeks

Social sciences criteria : Impact of the participation in the trial on participant quality of life and quality of sexual life

Through statistical analyses of some self-administered questionnaires items (in particular the SF12.v2 scale for quality of life) and thematic analyses of semi-directive individual interviews we will highlight the impact of the participation in the trial.

Time frame: from date of inclusion to the last follow-up visit date, up to 148 weeks