An Efficacy and Safety Study of Alirocumab in Children and Adolescents With Heterozygous Familial Hypercholesterolemia

Part of paid clinical trials in Boca Raton, Florida.

Sponsor: Sanofi
Study ID: NCT03510884
Phase: PHASE3
Status: Completed

Conditions

Hypercholesterolaemia

Eligibility Criteria

Sex: ALL
Age: 8 Years - 17 Years
Healthy Volunteers: Not accepted

Interventions

Alirocumab SAR236553 (REGN727) — DRUG
Pharmaceutical form:solution Route of administration: subcutaneous injection
Rosuvastatin — DRUG
Pharmaceutical form:tablet Route of administration: oral
Atorvastatin — DRUG
Pharmaceutical form:Tablet Route of administration: Oral
Simvastatin — DRUG
Pharmaceutical form:Tablet Route of administration: Oral
Pravastatin — DRUG
Pharmaceutical form:Tablet Route of administration: Oral
Lovastatin — DRUG
Pharmaceutical form:Tablet Route of administration: Oral
Fluvastatin — DRUG
Pharmaceutical form:Capsule Route of administration: Oral
Ezetimibe — DRUG
Pharmaceutical form:Tablet Route of administration: Oral
Cholestyramine — DRUG
Pharmaceutical form:oral suspension Route of administration: oral
Nicotinic acid — DRUG
Pharmaceutical form:Tablet Route of administration: Oral
Fenofibrate — DRUG
Pharmaceutical form:Tablet Route of administration: Oral
Omega-3 fatty acids — DRUG
Pharmaceutical form:capsule Route of administration: oral
Placebo — DRUG
Pharmaceutical form:solution Route of administration: subcutaneous injection

Study Details

Primary Objective: To evaluate the efficacy of alirocumab administered every 2 weeks (Q2W) and every 4 weeks (Q4W) versus placebo after 24 weeks of double-blind (DB) treatment on low-density lipoprotein cholesterol (LDL-C) levels in participants with heterozygous familial hypercholesterolemia (heFH) 8 to 17 years of age on optimal stable daily dose of statin therapy ± other lipid modifying therapies (LMTs) or a stable dose of non-statin LMTs in case of intolerance to statins. Secondary Objectives: * To evaluate the efficacy of alirocumab versus placebo on LDL-C levels. * To evaluate the effects of alirocumab versus placebo on other lipid parameters. * To evaluate the safety and tolerability of alirocumab in comparison with placebo. * To evaluate the efficacy, safety, and tolerability of alirocumab after open label treatment. * To evaluate the development of anti-alirocumab antibodies.

Key Dates

Start date: May 31, 2018
Status verified: Apr 2023
Primary completion: Jan 14, 2021
Completion: Aug 5, 2022

Study Design

Enrollment: 153 participants (actual)
Allocation: RANDOMIZED
Intervention model: PARALLEL
Primary purpose: TREATMENT

Arms

Experimental: Placebo/Alirocumab Q2W
Participants received subcutaneous (SC) injection of placebo (matched to alirocumab) based on their body weight (BW) (less than \[\<\] 50 kilograms \[kg\] or greater than or equal to \[\>=\] 50 kg) Q2W for 24 weeks in DB treatment period added to stable LMT. After completion of DB treatment period, eligible participants entered into OL treatment period and received alirocumab 40 milligrams (mg) (for BW \<50 kg) or 75 mg (for BW \>=50 kg) Q2W from Week 24 up to an additional 80 weeks (i.e., up to Week 104) added to stable LMT. After Week 24, dose up-titrated from 40 mg to 75 mg when BW increased from \<50 kg to \>=50 kg. From Week 32 up to Week 104, based on participant LDL-C value, alirocumab dose was either up-titrated as 40 mg to 75 mg (for BW \<50 kg) or 75 mg to 150 mg (for BW \>=50 kg) or down titrated as 75 mg to 40 mg (for BW \<50 kg) or 150 mg to 75 mg (for BW \>=50 kg).
Experimental: Alirocumab Q2W
Participants received SC injection of alirocumab 40 mg (for BW \<50 kg) or 75 mg (for BW \>=50 kg) Q2W for 24 weeks in DB treatment period added to stable LMT. Alirocumab dose was up-titrated to 75 mg or 150 mg Q2W from Week 12, when LDL-C level was \>=110 milligrams per deciliter (mg/dL) (2.85 millimoles per liter \[mmol/L\]) at Week 8. After completion of DB treatment period, eligible participants entered into OL treatment period and received alirocumab 40 mg (for BW \<50 kg) or 75 mg (for BW \>=50 kg) from Week 24 up to an additional 80 weeks (i.e., up to Week 104) added to stable LMT. After Week 24, dose up-titrated from 40 mg to 75 mg when BW increased from \<50 kg to \>=50 kg. From Week 32 up to Week 104, based on participant LDL-C value, alirocumab dose was either up-titrated as 40 mg to 75 mg (for BW \<50 kg) or 75 mg to 150 mg (for BW \>=50 kg) or down titrated as 75 mg to 40 mg (for BW \<50 kg) or 150 mg to 75 mg (for BW \>=50 kg).
Experimental: Placebo/Alirocumab Q4W
Participants received SC injection of placebo (matched to alirocumab) based on their BW (\<50 kg or \>=50 kg) Q4W for 24 weeks in DB treatment period added to stable LMT. After completion of DB treatment period, eligible participants entered into OL treatment period and received alirocumab 150 mg (for BW \<50 kg) or 300 mg (for BW \>=50 kg) Q4W from Week 24 up to an additional 80 weeks (i.e., up to Week 104) added to stable LMT. After Week 24, dose up-titrated from 150 mg to 300 mg when BW increased from \<50 kg to \>=50 kg. From Week 32 up to Week 104, based on participant LDL-C value, alirocumab dose was either up-titrated as 150 mg Q4W to 75 mg Q2W (for BW \<50 kg) or 300 mg Q4W to 150 mg Q2W (for BW \>=50 kg) or down titrated as 75 mg Q2W to 40 mg Q2W (for BW \<50 kg) or 150 mg Q2W to 75 mg Q2W (for BW \>=50 kg).
Experimental: Alirocumab Q4W
Participants received SC injection of alirocumab 150 mg (for BW \<50 kg) or 300 mg (for BW \>=50 kg) Q4W for 24 weeks in DB treatment period added to stable LMT. Alirocumab dose was up-titrated to 75 mg or 150 mg Q2W from Week 12, when LDL-C level \>=110 mg/dL (2.85 mmol/L) at Week 8. After completion of DB treatment period, eligible participants entered into OL treatment period and received alirocumab 150 mg (for BW \<50 kg) or 300 mg (for BW \>=50 kg) from Week 24 up to an additional 80 weeks (i.e., up to Week 104) added to stable LMT. After Week 24, dose up-titrated from 150 mg to 300 mg when BW increased from \<50 kg to \>=50 kg. From Week 32 up to Week 104, based on participant LDL-C value, alirocumab dose was either up-titrated as 150 mg Q4W to 75 mg Q2W (for BW \<50 kg) or 300 mg Q4W to 150 mg Q2W (for BW \>=50 kg) or down titrated as 75 mg Q2W to 40 mg Q2W (for BW \<50 kg) or 150 mg Q2W to 75 mg Q2W (for BW \>=50 kg).

Primary Outcome Measure

DB Period: Percent Change From Baseline in Low Density Lipoprotein Cholesterol (LDL-C) at Week 24: Intent-to-treat (ITT) Estimand [ Time Frame: Baseline, Week 24 ]

Locations (5)

Facility	City	State	ZIP	Site coordinators
Excel Medical Clinical Trials, LLC-Site Number:8400001	Boca Raton	Florida	33434	-
Washington University School of Medicine-Site Number:8400006	St Louis	Missouri	63110	-
Presbyterian Novant Heart & Wellness-Site Number:8400002	Charlotte	North Carolina	28204	-
Cincinnati Children's Hospital Medical Center-Site Number:8400005	Cincinnati	Ohio	45229	-
Vanderbilt University-Site Number:8400003	Nashville	Tennessee	37232	-

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Excel Medical Clinical Trials, LLC· Boca Raton, FL Washington University School of Medicine· St Louis, MO Presbyterian Novant Heart & Wellness· Charlotte, NC Cincinnati Children's Hospital Medical Center· Cincinnati, OH Vanderbilt University· Nashville, TN

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