HIV-1-infection Clinical Trial
Official title:
Changes in Immunologic Parameters Following the Addition of Fostemsavir in Virologically Suppressed Immunologic Non-responders Living With HIV-the RECOVER Study
The RECOVER study is a self-controlled case series to evaluate whether the addition of Fostemsavir (Rukobia) to a stable HIV regimen in virologically suppressed patients living with HIV who never experience optimal CD4 T-cell count recovery can result in meaningful increases in different immunologic parameters such as CD4 T-cell count, CD4 T-cell percentage and CD4/CD8 ratio
Status | Recruiting |
Enrollment | 50 |
Est. completion date | August 31, 2024 |
Est. primary completion date | July 31, 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years to 65 Years |
Eligibility | Inclusion Criteria: - HIV-1 infected men or women - Aged 18-65 - Stable insurance plan - Documented plasma HIV-1 RNA < 50 c/mL x 2 within the last year prior to screening - Must be on a stable ARV regimen for =6 months prior to screening - CD4+T-cell count<350 cells/mm3 while on ARVs for at least 2 years - Must be willing to add FTR 600 mg twice daily to their current antiretroviral regimen - Must have attended = 2 clinic visits in the 12 months prior to screening Exclusion Criteria: - Newly or recently diagnosed HIV-1 infection defined as HIV-1 infection diagnosed in the prior 6 months - Active HBV or HCV co-infection - Unstable liver disease or Child-Pugh C liver disease - History of autoimmune disease - History of any malignancy =5 years - History of radiation or cytotoxic chemotherapy - Use of systemic corticosteroids or other immunomodulatory agents in the last 14 days prior to study entry - Confirmed QT value > 500 msec at Screening or Day 1 or confirmed QTcF value > 470 msec for women and > 450 msec for men at Screening or Day 1 |
Country | Name | City | State |
---|---|---|---|
United States | Orlando Immunology Center | Orlando | Florida |
Lead Sponsor | Collaborator |
---|---|
Orlando Immunology Center | ViiV Healthcare |
United States,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Other | Impact of fostemsavir treatment on inflammatory, cellular functional, and viral reservoir biomarkers in immunologic non responders | Weeks 24 and 48 | ||
Other | Identification of biomarkers that may predict CD4 recovery and Immunologic non response | Weeks 24 and 48 | ||
Other | Evaluation of gp120 detection and correlation with reservoir and inflammatory biomarkers | Weeks 24 and 48 | ||
Primary | Mean and median change in CD4+T-cell count | mean and median change in CD4+T-cell count after the addition of fostemsavir to baseline ARV regimens in virologically suppressed immunologic non responders using pre-fostemsavir values as controls | 48 weeks | |
Secondary | Mean and median change in CD4+T-cell count | mean and median change in CD4+T-cell count after the addition of fostemsavir to baseline ARV regimens in virologically suppressed immunologic non responders using pre-fostemsavir values as controls | 24 weeks | |
Secondary | mean and median change in CD4+T-cell count percentage | mean and median change in CD4+ percentage after the addition of fostemsavir to baseline ARV regimens in virologically suppressed immunologic non responders using pre-fostemsavir values as controls | 24 and 48 weeks | |
Secondary | mean and median change in CD4/CD8 ratio | mean and median change in CD4/CD8 ratio after the addition of fostemsavir to baseline ARV regimens in virologically suppressed immunologic non responders using pre-fostemsavir values as controls | 24 and 48 weeks | |
Secondary | Proportion with virologic failure defined as an HIV-1 RNA=50 c/mL | proportion of patients with HIV-1 RNA =50 c/mL after the addition of fostemsavir to baseline ARV regimens in virologically suppressed immunologic non responders using pre-fostemsavir values as controls | 24 and 48 weeks | |
Secondary | Safety and tolerability of fostemsavir | Incidence and severity of AEs and laboratory abnormalities and proportion of subjects who discontinue treatment due to AEs | Weeks 24 and 48 | |
Secondary | Change in concomitant medications after adding fostemsavir to the baseline ARV regimen over time | Change in number of concomitant medications after the addition of fostemsavir to the baseline ARV regimen using number of concomitant medications pre-fostemsavir as the comparator | Weeks 24 and 48 | |
Secondary | Impact of adding fostemsavir to the baseline ARV regimen on medications needed for OI prophylaxis over time | Change in number of concomitant medications for OI prophylaxis after the addition of fostemsavir to the baseline ARV regimen using number of concomitant medications for OI prophylaxis pre-fostemsavir as the comparator | Weeks 24 and 48 | |
Secondary | Impact of adding fostemsavir to the baseline ARV regimen on OI incidence and severity over time | Proportion of patients with an incident OI and Change in the severity of incident OIs (grading using the DAIDS grading table) | Weeks 24 and 48 | |
Secondary | Assessment of health related quality of life after the addition of fostemsavir to baseline ARV regimens | Change from Baseline in QOL scores using the WHOQOL-HIV BREF | Weeks 24 and 48 | |
Secondary | Assessment of HIV or ART-related symptoms after the addition of fostemsavir to baseline ARV regimen | Change from Baseline in health status score using the HIV-SI (HIV-Symptom Index) | Weeks 24 and 48 | |
Secondary | Assessment of treatment satisfaction in subjects who have fostemsavir added to their baseline ARV regimen | Change from baseline in treatment satisfaction using the HIV TSQs questionnaire | Weeks 24 and 48 | |
Secondary | Assessment of viral resistance in subjects meeting Virologic Rebound Criteria | Incidence of observed genotypic resistance to ARVs for subjects meeting Virologic Rebound Criteria | Weeks 24 and 48 |
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