HIV Infections Clinical Trial
— MAFALDA-ROfficial title:
An Open Label, Comparative, Randomized , Phase IV Pilot Study to Evaluate the Efficacy and Safety of a Rilpivarine-based Antiretroviral Tratment Regimen in HIV- Infected Patients With Liver Metabolic Disease Who Maintain Udetectable HIV Viral Load
Verified date | June 2023 |
Source | Fundacion SEIMC-GESIDA |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
In HIV-infected people with metabolic fatty liver disease and liver fibrosis of any degree, as measured by non-invasive testing, antiretroviral treatment that includes rilpivinire for 18 months results in a slowing of progression and/or reduction of fatty metabolic liver disease, attenuating inflammation and liver fibrosis.
Status | Active, not recruiting |
Enrollment | 75 |
Est. completion date | April 1, 2025 |
Est. primary completion date | November 1, 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: - Patients over 18 years of age with HIV infection who have never received antiretroviral treatment with Rilpivirine. - Have a stable ART pattern for at least the last 6 month Exclusion Criteria: - Not having received more than three previous lines of antiretroviral treatment - No resistance mutations that compromise the efficacy of Rilpivirine, Dolutegravir, Tenofovir (TDF and/or TAF) or Emtricitabine. - Have an HIV viral load < 50 copies/ml for at least the last 6 months, 1 blip below 500 copies/ml is allowed during this period. - Have an ultrasound-diagnosed fatty liver metabolic disease or a CAP (Controlled Attenuation Parameter®) measurement > 238 dB/m with an IQR < 30 dB/m. - Have an fatty liver metabolic disease with some degree of fibrosis diagnosed by ET (Fibroscan®) > 5.2 kPa. In patients in whom ET is not possible, have a FIB-4 >1.3. - Be able to understand and comply with the requirements and instructions of the protocol. - Understanding long-term commitment to study - Acceptance of their participation in the study by signing an informed consent form. Exclusion Criteria: - Have chronic HBV infection (presence of HBsAg+) or HCV (detectable HCV viral load). Patients with past treated HCV are also not allowed to be included (does not include patients with spontaneously resolved HCV infection). - Have diabetes mellitus on treatment with SGLT2, GLP1 or plioglitazone of less than 6 months duration. - Have a history of alcohol abuse - Harmful alcohol consumption, defined as >30 grams of alcohol per day in men and >20 grams of alcohol per day in women. - Have chronic decompensated liver disease, defined as any of the following: presence of encephalopathy, ascites, coagulopathy, oesophageal or gastric varices, or persistent jaundice. - Any previous physical or mental condition (such as habitual drug use) that the investigator believes may interfere with the patient's ability to comply with the study protocol. - Pregnancy or breastfeeding at the screening visit or at any time during the study or intention to become pregnant during the study period. - Prior history of Rilpivirine use of any duration. |
Country | Name | City | State |
---|---|---|---|
Spain | Hospital Universitario Gregorio Marañon | Madrid | |
Spain | Hospital universitario Infanta Leonor | Madrid | |
Spain | Hospital Universitario Infanta Sofía | Madrid | |
Spain | Hospital Universitario La Paz | Madrid |
Lead Sponsor | Collaborator |
---|---|
Fundacion SEIMC-GESIDA |
Spain,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | To evaluate the efficacy of Rilpivirine (RPV) as part of the antiretroviral treatment regimen in VIH-infected people, to slow the progression and/or reduce liver fibrosis of any degree | To measure the no progression and/or regression of liver fibrosis:
No change in liver stiffness as measured by ET (Transient Elastography) or FIB4 at the 18-month visit with respect to the baseline, the intervention group (branches 1 and 2) compared to the control group. |
18 months | |
Primary | To evaluate the efficacy of Rilpivirine (RPV) as part of the antiretroviral treatment regimen in VIH-infected people, to slow the progression and/or reduce liver fibrosis of any degree | Reduction in liver stiffness measured by ET or FIB4 at the 18-month visit from baseline in the intervention group (arms 1 and 2) versus the control group. | 18 months | |
Secondary | Efficacy of RPV in reducing liver fibrosis of any grade | To evaluate the efficacy of RPV in reducing liver fibrosis of any grade, as measured by non-invasive tests, in HIV-infected people:
as part of a nucleoside analogue-free antiretroviral treatment regimen as part of an antiretroviral treatment regimen that includes tenofovir Proportion of subjects with ET measurement < 5.2 kPa in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months from the start of treatment. |
12-18 months | |
Secondary | Efficacy of RPV in reducing liver fibrosis of any grade | Proportion of subjects with a FIB4 measurement < 1.3 in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months from the start of treatment. | 12-18 months | |
Secondary | Efficacy of RPV in reducing liver fibrosis of any grade | The mean reduction in the APRI measure in the intervention group (arms 1 and 2) versus the control group at 12 and 18 months after the start of treatment. | 12-18 months | |
Secondary | Efficacy of RPV in reducing liver fibrosis of any grade | Proportion of subjects with an APRI measure < 0.5 in the intervention group (arms 1 and 2) versus the control group at 12 and 18 months from the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | The mean reduction in the percentage of liver fat, measured by magnetic resonance imaging, which measures the proton density fraction of fat (MRI-PDFF), between the beginning and the end of the study comparing the intervention group (arms 1 and 2) vs control group | 18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | Difference in the proportion of responders between the intervention group (arms 1 and 2) at 18 months from the start of treatment, defined as those who achieve >30% reduction in hepatic steatosis measured by MRI-PDFF | 18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | Proportion of subjects with hepatic steatosis measured as MRI-PDFF > 5% steatosis in the intervention group (arms 1 and 2) compared to the control group at 18 months from the start of treatment | 18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | The mean reduction of the CAP measurement in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | The mean reduction in the FLI measurement in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | The mean reduction in the HSI measure in the intervention group (arms 1 and 2) versus the control group at 12 and 18 months from the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | The mean reduction of the TyG measurement in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | Proportion of subjects with hepatic steatosis measured as CAP > 238 dB/m in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months from the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | The mean reduction in the FLI measurement in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | Proportion of subjects with hepatic steatosis measured as HSI score > 36 in the intervention group (arms 1 and 2) versus the control group at 12 and 18 months from the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to reduce hepatic steatosis | Proportion of subjects with hepatic steatosis measured as TyG score > 8.38 in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months from the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the insulin resistance | The mean reduction of the HOMA-IR value in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the insulin resistance | Difference in the proportion of subjects with insulin resistance, measured as HOMA-IR >2.5 in the intervention group (arms 1 and 2) versus the control group at 12 and 18 months after the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the insulin resistance | Mean reduction in TyG (IR) measurement in the intervention group (arms 1 and 2) versus the control group at 12 and 18 months from the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the insulin resistance | Difference in the proportion of subjects with insulin resistance measured as TyG > 4.68 in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months from the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the insulin resistance | The mean reduction in fasting blood glucose (mg/dL) in the intervention group (arms 1 and 2) versus the control group at 12 and 18 months from the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the insulin resistance | Difference in the proportion of subjects with fasting glycemia > 100 mg/dL in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the insulin resistance | The reduction in the measurement of abdominal circumference and waist ratio/in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatmen | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to improve the lipid metabolism | The mean reduction in fasting triglycerides (mg/dL) in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to improve the lipid metabolism | Difference in the proportion of subjects with hypertriglyceridemia (value > 150 mg/dL) in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to improve the lipid metabolism | Mean reduction in fasting LDL cholesterol quantification (mg/dL) in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to improve the lipid metabolism | Difference in the proportion of subjects with elevated LDL cholesterol (value > 130 mg/dL and value >100 mg/dL) in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months of start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to improve the lipid metabolism | The mean increase in fasting HDL cholesterol quantification (mg/dL) in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to improve the lipid metabolism | Difference in the proportion of subjects with elevated HDL cholesterol (value > 45 mg/dL in men and value > 50 mg/dL in women) in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months from the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to improve the lipid metabolism | The mean reduction in fasting non-LDL cholesterol quantification (mg/dL) in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment. | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to improve the lipid metabolism | Difference in the proportion of subjects with elevated non-LDL cholesterol (value > 160 mg/dL) in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months after the start of treatment | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the liver inflammation | The mean change in ALT value (IU/mL) in the intervention group (arms 1 and 2) vs. the control group at 12 and 18 months from baseline | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the liver inflammation | The mean change in AST value (IU/mL) in the intervention group (arms 1 and 2) versus the control group at 12 and 18 months from the baseline visit | 12-18 months | |
Secondary | To evaluate the efficacy of Rilpivirine (RPV) to decrease the liver inflammation. | The change of the gene expression value of: IL1-beta, IL6, IL10, MCP1, PAI-1, TGF-alpha, TNF-alpha in PBMCs in the intervention group (arms 1 and 2) compared to the control group at 12 and 18 months compared to the baseline visit. | 12-18 months | |
Secondary | Efficacy of RPV to reduce hepatic steatosis/fibrosis. | To assess the efficacy of RPV as part of the antiretroviral treatment regimen in HIV-infected individuals to reduce hepatic steatosis/fibrosis based on the presence of PNPLA3 and MBOAT7-TMC4 genetic polymorphisms. | 18 months | |
Secondary | To characterise the effects of RPV on the expression of inflammatory and fibrogenic markers in peripheral blood mononuclear cells | . Analyse the gene expression of inflammatory and fibrogenic markers in peripheral blood polymorphonuclear cells by RT-PCR: IL1-gamma, IL6, IL10, MCP1, P AI-1, TGF-beta, TNF-alpha. | 18 months | |
Secondary | To characterise the effects of RPV on the expression of inflammatory and fibrogenic markers in peripheral blood mononuclear cells | . Measurement of ALT, AST and GGT in plasma as markers of inflammation. | 18 months | |
Secondary | Efficacy of RPV to reduce the progression to steatohepatitis | In previous studies it has shown that PNPLA3, TM6SF2, and MBOAT7-TMC4 polymorphisms are associated with elevated ALT levels and histologic parameters of nonalcoholic steatohepatitis and fibrosis severity.
On the baseline visit will be collected biological samples for genetuic study. A 3 ml blood sample will be drawn into an EDTA tube at baseline visit for determination of PNPLA3 (C, G alleles) and MBOAT7-TMC4 (G, A alleles) genetic polymorphisms. |
18 months |
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