Efficacy and Safety of a Microsomal Triglyceride Transfer Protein Inhibitor in Patients with Homozygous Familial Hypercholesterolaemia: a Single-arm, Open-label, Phase 3 Study

Overview

Journal Lancet

Publisher Elsevier

Specialty General Medicine

Date 2012 Nov 6

PMID 23122768

Citations 228

Authors

Marina Cuchel

Emma A Meagher

Hendrik du Toit Theron

Dirk J Blom

A David Marais

Robert A Hegele

Maurizio R Averna

Cesare R Sirtori

Prediman K Shah

Daniel Gaudet

Claudia Stefanutti

Giovanni B Vigna

Anna M E Du Plessis

Kathleen J Propert

William J Sasiela

LeAnne T Bloedon

Daniel J Rader

Affiliations

Soon will be listed here.

Abstract

Background: Patients with homozygous familial hypercholesterolaemia respond inadequately to existing drugs. We aimed to assess the efficacy and safety of the microsomal triglyceride transfer protein inhibitor lomitapide in adults with this disease.

Methods: We did a single-arm, open-label, phase 3 study of lomitapide for treatment of patients with homozygous familial hypercholesterolemia. Current lipid lowering therapy was maintained from 6 weeks before baseline through to at least week 26. Lomitapide dose was escalated on the basis of safety and tolerability from 5 mg to a maximum of 60 mg a day. The primary endpoint was mean percent change in levels of LDL cholesterol from baseline to week 26, after which patients remained on lomitapide through to week 78 for safety assessment. Percent change from baseline to week 26 was assessed with a mixed linear model.

Findings: 29 men and women with homozygous familial hypercholesterolaemia, aged 18 years or older, were recruited from 11 centres in four countries (USA, Canada, South Africa, and Italy). 23 of 29 enrolled patients completed both the efficacy phase (26 weeks) and the full study (78 weeks). The median dose of lomitapide was 40 mg a day. LDL cholesterol was reduced by 50% (95% CI -62 to -39) from baseline (mean 8·7 mmol/L [SD 2·9]) to week 26 (4·3 mmol/L [2·5]; p<0·0001). Levels of LDL cholesterol were lower than 2·6 mmol/L in eight patients at 26 weeks. Concentrations of LDL cholesterol remained reduced by 44% (95% CI -57 to -31; p<0·0001) at week 56 and 38% (-52 to -24; p<0·0001) at week 78. Gastrointestinal symptoms were the most common adverse event. Four patients had aminotransaminase levels of more than five times the upper limit of normal, which resolved after dose reduction or temporary interruption of lomitapide. No patient permanently discontinued treatment because of liver abnormalities.

Interpretation: Our study suggests that treatment with lomitapide could be a valuable drug in the management of homozygous familial hypercholesterolaemia.

Funding: FDA Office of the Orphan Product Development, Aegerion Pharmaceuticals.

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