Long-term Efficacy of Lipoprotein Apheresis and Lomitapide in the Treatment of Homozygous Familial Hypercholesterolemia (HoFH): a Cross-national Retrospective Survey

Overview

Journal Orphanet J Rare Dis

Publisher Biomed Central

Specialty General Medicine

Date 2021 Sep 9

PMID 34496902

Citations 11

Authors

Laura DErasmo

Antonio Gallo

Angelo Baldassare Cefalu

Alessia Di Costanzo

Samir Saheb

Antonina Giammanco

Maurizio Averna

Alessio Buonaiuto

Gabriella Iannuzzo

Giuliana Fortunato

Arturo Puja

Tiziana Montalcini

Chiara Pavanello

Laura Calabresi

Giovanni Battista Vigna

Marco Bucci

Katia Bonomo

Fabio Nota

Tiziana Sampietro

Francesco Sbrana

Patrizia Suppressa

Carlo Sabba

Fabio Fimiani

Arturo Cesaro

Paolo Calabro

Silvia Palmisano

Sergio DAddato

Livia Pisciotta

Stefano Bertolini

Randa Bittar

Olga Kalmykova

Sophie Beliard

Alain Carrie

Marcello Arca

Eric Bruckert

Affiliations

Soon will be listed here.

Abstract

Background: Homozygous familial hypercholesterolemia (HoFH) is a rare life-threatening condition that represents a therapeutic challenge. The vast majority of HoFH patients fail to achieve LDL-C targets when treated with the standard protocol, which associates maximally tolerated dose of lipid-lowering medications with lipoprotein apheresis (LA). Lomitapide is an emerging therapy in HoFH, but its place in the treatment algorithm is disputed because a comparison of its long-term efficacy versus LA in reducing LDL-C burden is not available. We assessed changes in long-term LDL-C burden and goals achievement in two independent HoFH patients' cohorts, one treated with lomitapide in Italy (n = 30) and the other with LA in France (n = 29).

Results: The two cohorts differed significantly for genotype (p = 0.004), baseline lipid profile (p < 0.001), age of treatment initiation (p < 0.001), occurrence of cardiovascular disease (p = 0.003) as well as follow-up duration (p < 0.001). The adjunct of lomitapide to conventional lipid-lowering therapies determined an additional 58.0% reduction of last visit LDL-C levels, compared to 37.1% when LA was added (p = 0.004). Yearly on-treatment LDL-C < 70 mg/dl and < 55 mg/dl goals were only achieved in 45.5% and 13.5% of HoFH patients treated with lomitapide. The long-term exposure to LDL-C burden was found to be higher in LA than in Lomitapide cohort (13,236.1 ± 5492.1 vs. 11,656.6 ± 4730.9 mg/dL-year respectively, p = 0.002). A trend towards fewer total cardiovascular events was observed in the Lomitapide than in the LA cohort.

Conclusions: In comparison with LA, lomitapide appears to provide a better control of LDL-C in HoFH. Further studies are needed to confirm this data and establish whether this translates into a reduction of cardiovascular risk.

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