HIV Infections Clinical Trial
— RALAM-IIOfficial title:
Phase 3b, Single Arm, Simplification Study With Dual Therapy Including Lamivudine (300 mg QD) Plus Raltegravir (1200 mg QD) in Virologically Suppressed HIV-1 Infected Patients Experiencing Inconvenience, Toxicity, Negative Impact on Co-morbidities or Risk of Drug-drug Interactions With Their Current Regimen. RALAM-II Study
Phase 3b, single arm, simplification study with dual therapy including Lamivudine (300 mg QD) plus Raltegravir (1200 mg QD) in virologically suppressed HIV-1 infected patients experiencing inconvenience, toxicity, negative impact on comorbidities or risk of drug-drug interactions with their current regimen.
Status | Recruiting |
Enrollment | 50 |
Est. completion date | March 30, 2020 |
Est. primary completion date | March 30, 2020 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility |
Inclusion Criteria: - Eligible patients will be males or females at least 18 years of age. Women of childbearing potential must have a negative pregnancy test within 10 days prior to randomization into the study. - Patients seropositive for HIV-1 using standard diagnostic criteria. - Patients experiencing inconvenience, toxicity, negative impact on comorbidities or risk of drug-drug interactions with their current regimen - Patients virologically suppressed during at least 12 months prior to inclusion (viral load <50 copies/mL). - Patients who have signed informed consent to participate in the study. Exclusion Criteria: - Pregnancy, lactation, or planned pregnancy during the study period. - Previous failure to an integrase inhibitor-containing regimen. - Previous failure to a Lamivudine or Emtricitabine-containing regimen. - Resistance mutations to Lamivudine or integrase inhibitor if any resistance test had been previously performed. - Any disease or history of disease which, in the opinion of the investigator, might confound the results of the study or pose additional risk to patient treatment. - Chronic hepatitis B. |
Country | Name | City | State |
---|---|---|---|
Spain | Hospital Clínic i Provincial de Barcelona | Barcelona |
Lead Sponsor | Collaborator |
---|---|
David Garcia Cinca | Fundacion Clinic per a la Recerca Biomédica |
Spain,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Therapeutic failure | therapeutic failure at week 48, includes virological failure, change in treatment for any reason, consent withdrawal, loss to follow-up or death | 48 weeks | |
Secondary | Change from baseline in the reason of change of the antiretroviral treatment in those patients the reason of change was inconenience | Changes in quality of life calculated by EQ-5D-5L if reason of switch was inconvenience | 48 weeks | |
Secondary | Change from baseline in the reason of change of the antiretroviral treatment in those patients the reason of change was neurological toxicity | Changes on Pittsburgh Sleep Quality Index for neurological toxicity | 48 weeks | |
Secondary | Change from baseline in the reason of change of the antiretroviral treatment in those patients the reason of change was cardiovascular toxicity or co-morbidity | Changes on plasma lipids cholesterol LDL | 48 weeks | |
Secondary | Change from baseline in the reason of change of the antiretroviral treatment in those patients the reason of change was cardiovascular toxicity or co-morbidity | Changes on plasma lipids cholesterol HDL | 48 weeks | |
Secondary | Change from baseline in the reason of change of the antiretroviral treatment in those patients the reason of change was cardiovascular toxicity or co-morbidity | Changes on plasma lipids triglycerides | 48 weeks | |
Secondary | Change from baseline in the reason of change of the antiretroviral treatment in those patients the reason of change was skeletal toxicity | Changes on dual energy x-ray absorptiometry bone density | 48 weeks | |
Secondary | Change from baseline in the reason of change of the antiretroviral treatment in those patients the reason of change was digestive toxicity | Apperance of any adverse event that resolve their digestive toxicity: as diarrhea or digestive discomfort | 48 weeks | |
Secondary | Change from baseline in the reason of change of the antiretroviral treatment in those patients the reason of change was drug-drug interactions | Proportion of drug-drug interaction with antirretroviral treatment | 48 weeks | |
Secondary | Therapeutic failure | 24 weeks | ||
Secondary | Virological failure | Defined as two consecutive measurements of plasma viral load above 50 copies/ml | 24 weeks | |
Secondary | Virological failure | Defined as two consecutive measurements of plasma viral load above 50 copies/ml | 48 weeks | |
Secondary | Proportion of patients with viral load below ultrasensitive HIV-1 RNA detection limit (limit of detection 1 copy/mL) | 48 weeks | ||
Secondary | Changes from baseline in cholesterol total | 24 weeks | ||
Secondary | Changes from baseline in HDL | 24 weeks | ||
Secondary | Changes from baseline in triglycerides | 24 weeks | ||
Secondary | Changes from baseline in insulin resistance (HOMA-IR) | 24 weeks | ||
Secondary | Changes from baseline in cholesterol LDL | 24 weeks | ||
Secondary | Changes from baseline in cholesterol LDL | 48 weeks | ||
Secondary | Changes from baseline in cholesterol total | 48 weeks | ||
Secondary | Changes from baseline in cholesterol HDL | 48 weeks | ||
Secondary | Changes from baseline in triglycerides | 48 weeks | ||
Secondary | Changes from baseline in and insulin resistance (HOMA-IR) | 48 weeks | ||
Secondary | Changes from baseline in body fat composition | 48 weeks | ||
Secondary | Changes from baseline in immune activation markers including CD38 | 48 weeks | ||
Secondary | Changes from baseline in immune activation markers including HLA-DR | 48 weeks | ||
Secondary | Changes from baseline in biomarkers of inflammation IL-6, | 48 weeks | ||
Secondary | Changes from baseline in biomarkers of inflammation high sensitivity C-reactive protein | 48 weeks | ||
Secondary | Changes from baseline in biomarkers of mononuclear activation SD-14 | 48 weeks | ||
Secondary | Changes from baseline in biomarkers of mononuclear activation SD-163 | 48 weeks | ||
Secondary | Changes from baseline in sleep quality (Pittsburgh Sleep Quality Index) | 24 weeks | ||
Secondary | Changes from baseline in sleep quality (Pittsburgh Sleep Quality Index) | 48 weeks | ||
Secondary | Change from baseline in EQ-5D-5L | 24 weeks | ||
Secondary | Change from baseline in EQ-5D-5L | 48 weeks | ||
Secondary | Incidence of adverse events | 48 weeks |
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