Familial Partial Lipodystrophy Clinical Trial
— LEAPOfficial title:
A Randomized Double-Blind Placebo-Controlled Study of the LEPR Agonist Antibody REGN4461 for the Treatment of Metabolic Abnormalities in Patients With Familial Partial Lipodystrophy
Verified date | June 2024 |
Source | Regeneron Pharmaceuticals |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
Two cohorts are being studied based on leptin levels. Cohort A is composed of patients with baseline leptin <8.0 ng/mL and Cohort B is composed of patients with baseline leptin 8.0 to ≤20.0 ng/mL The primary objectives will be evaluated for patients in Cohort A only: - To evaluate the effect of REGN4461 on fasting triglycerides (TG) in patients with elevated baseline fasting TG - To evaluate the effect of REGN4461 on hyperglycemia in patients with elevated baseline Hemoglobin A1c (HbA1c) The following secondary objectives of the study will be evaluated for Cohort B and for the combined set of Cohorts A plus B: - To evaluate the effect of REGN4461 on fasting TG levels in patients with hypertriglyceridemia - To evaluate the effect of REGN4461 on glycemic control in patients with hyperglycemia The following secondary objectives of the study will be evaluated for Cohorts A and B separately, and for the combined set of Cohorts A plus B: - To evaluate the effect of REGN4461 on liver fat in patients with hepatic steatosis - To evaluate the effect of REGN4461 on hunger - To evaluate safety and tolerability of REGN4461 - To characterize the concentration profile of REGN4461 over time - To assess immunogenicity to REGN4461
Status | Terminated |
Enrollment | 20 |
Est. completion date | April 18, 2024 |
Est. primary completion date | October 31, 2023 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Key Inclusion Criteria: - Clinical diagnosis of familial partial lipodystrophy as defined in the protocol - Fasting leptin level =20.0 ng/ml, as determined during the screening period - Presence of significant metabolic abnormalities related to glucose and triglycerides (TGs) as defined in the protocol - Stable body weight within the 3 months prior to screening (no gain or loss of >5% current weight) - Stable diet during the past 3 months defined as no major change in macronutrient composition (eg, starting or stopping diets such as Atkins, Paleo, Vegetarianism, Veganism) - No clinically meaningful change in medication regimen in the 3 months prior to screening as defined in the protocol Key Exclusion Criteria: - Treatment with metreleptin within 3 months of the screening visit - Patients with a diagnosis of generalized lipodystrophy - Patients with a diagnosis of acquired lipodystrophy - Pregnant or breastfeeding women NOTE: Other protocol defined inclusion/exclusion criteria apply |
Country | Name | City | State |
---|---|---|---|
France | ICAN, Institute of Cardiometabolism and Nutrition | Paris | |
Spain | Complexo Hospitalario Universitario de Santiago-Hospital Médico-Cirúrxico de Conxo | Santiago de Compostela | Galicia |
Turkey | Ege University Faculty of Medicine | Izmir | Bornova |
United States | University of Michigan | Ann Arbor | Michigan |
United States | National Institute of Health | Bethesda | Maryland |
United States | Excel Medical Clinical Trials - A Flourish Research Site | Boca Raton | Florida |
United States | UT Southwestern Medical Center | Dallas | Texas |
United States | University of Pittsburgh Medical Center | Pittsburgh | Pennsylvania |
Lead Sponsor | Collaborator |
---|---|
Regeneron Pharmaceuticals |
United States, France, Spain, Turkey,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Percent change in fasting serum triglyceride (TG) | In patients with elevated baseline fasting TG (fasting TG =200 mg/dL) and with baseline leptin <8.0 ng/mL | Baseline to week 12 | |
Primary | Absolute change in hemoglobin A1c (HbA1c) | In patients with elevated baseline HbA1c (>7.0%) and with baseline leptin <8.0 ng/mL | Baseline to week 12 | |
Secondary | Percent change in fasting serum TG | In patients with elevated baseline fasting TG (>200 mg/dL)
Cohort B and Cohorts A+B |
Baseline to week 12 | |
Secondary | Absolute change in HbA1c | In patients with elevated baseline HbA1c (>7.0%)
Cohort B and Cohorts A+B |
Baseline to week 12 | |
Secondary | Percent change in fasting serum TG | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Baseline to week 12 | |
Secondary | Percent change in fasting serum TG | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Week 12 to week 24 | |
Secondary | Percent change in fasting serum TG from baseline to week 12 compared to the percent change between week 12 and week 24 | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Week 24 | |
Secondary | Percent change in fasting serum TG | Cohorts A and B separately and Cohorts A+B in Study Arm 2 | Baseline to week 24 | |
Secondary | Percent change in fasting serum TG after the first 12 weeks of exposure to REGN4461 | Cohorts A and B separately and Cohorts A+B in Study Arm 2 | Baseline to week 12 | |
Secondary | Percent change in fasting serum TG after the first 12 weeks of exposure to REGN4461 | Cohorts A and B separately and Cohorts A+B in Study Arm 1 Patients must meet stability criteria | Week 12 to week 24 | |
Secondary | Change in HbA1c | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Baseline to week 12 | |
Secondary | Change in HbA1c | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Week 12 to week 24 | |
Secondary | Change in HbA1c from baseline to week 12 compared to change between week 12 and week 24 | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Week 24 | |
Secondary | Change in fasting glucose | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Baseline to week 12 | |
Secondary | Change in fasting glucose | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Week 12 to week 24 | |
Secondary | Change in fasting glucose from baseline to week 12 compared to change between week 12 and week 24 | Cohorts A and B separately and Cohorts A+B in Study Arm 1 | Week 24 | |
Secondary | Change in HbA1c | Cohorts A and B separately and Cohorts A+B in Study Arm 2 | Baseline to week 24 | |
Secondary | Change in fasting glucose | Cohorts A and B separately and Cohorts A+B in Study Arm 2 | Baseline to week 24 | |
Secondary | Change in HbA1c | Cohorts A and B separately and Cohorts A+B in Study Arm 2 | Baseline to week 12 | |
Secondary | Change in HbA1c | Cohorts A and B separately and Cohorts A+B in Study Arm 1 Patients must meet stability criteria | Week 12 to week 24 | |
Secondary | Change in fasting glucose | Cohorts A and B separately and Cohorts A+B in Study Arm 2 | Baseline to week 12 | |
Secondary | Percent change in liver fat magnetic resonance imaging-derived proton density fat fraction (MRI-PDFF) REGN4461 | In patients with baseline liver fat (MRI-PDFF) =8.5%
Cohorts A and B separately and Cohorts A+B |
Baseline to week 12 | |
Secondary | Percent change in liver fat (MRI-PDFF) placebo | In patients with baseline liver fat (MRI-PDFF) =8.5%
Cohorts A and B separately and Cohorts A+B |
Baseline to week 12 | |
Secondary | Percent change in liver fat (MRI-PDFF) REGN4461 versus placebo | In patients with baseline liver fat (MRI-PDFF) =8.5%
Cohorts A and B separately and Cohorts A+B |
Baseline to week 12 | |
Secondary | Percent change in liver fat (MRI-PDFF) | In patients with baseline liver fat (MRI-PDFF) =8.5%
Cohorts A and B separately and Cohorts A+B in Study Arm 1 |
Baseline to week 12 | |
Secondary | Percent change in liver fat (MRI-PDFF) | In patients with baseline liver fat (MRI-PDFF) =8.5%
Cohorts A and B separately and Cohorts A+B in Study Arm 1 |
Week 12 to week 24 | |
Secondary | Percent change in liver fat (MRI-PDFF) from baseline to week 12 compared to percent change between week 12 and week 24 | In patients with baseline liver fat (MRI-PDFF) =8.5%
Cohorts A and B separately and Cohorts A+B in Study Arm 1 |
Week 24 | |
Secondary | Percent change in liver fat (MRI-PDFF) | In patients with baseline liver fat (MRI-PDFF) =8.5%
Cohorts A and B separately and Cohorts A+B in Study Arm 2 |
Baseline to week 24 | |
Secondary | Percent change in liver fat (MRI-PDFF) | In patients with baseline liver fat (MRI-PDFF) =8.5%
Cohorts A and B separately and Cohorts A+B in Study Arm 2 |
Baseline to week 12 | |
Secondary | Change on the daily lipodystrophy hunger questionnaire | Cohorts A and B separately and Cohorts A+B
Patients will complete the PRO assessments daily. The Hunger questionnaire is self-administered and contains 4 items based on a Likert-like scale, where 0 is not hungry at all and 10 is the hungriest possible |
Baseline to week 12 | |
Secondary | Change on the daily lipodystrophy hunger questionnaire | Cohorts A and B separately and Cohorts A+B | Baseline to week 24 | |
Secondary | Incidence and severity of treatment-emergent adverse events (TEAEs) | Cohorts A and B separately and Cohorts A+B | Up to week 40 | |
Secondary | Concentrations of REGN4461 in serum over time | Cohorts A and B separately and Cohorts A+B | Up to week 40 | |
Secondary | Immunogenicity of REGN4461 over time compared to placebo | Cohorts A and B separately and Cohorts A+B | Up to week 40 |
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