Successful Reinstitution of Agalsidase Beta Therapy in Fabry Disease Patients with Previous IgE-antibody or Skin-test Reactivity to the Recombinant Enzyme

Overview

Journal Genet Med

Publisher Elsevier

Specialty Genetics

Date 2008 May 23

PMID 18496035

Citations 25

Authors

David Bodensteiner

C Ronald Scott

Katherine B Sims

Gillian M Shepherd

Rebecca D Cintron

Dominique P Germain

Affiliations

Soon will be listed here.

Abstract

Purpose: To determine if enzyme replacement therapy, involving intravenous infusions of recombinant human alpha-galactosidase A (agalsidase beta; Fabrazyme), could be safely continued in patients with Fabry disease who had been withdrawn from a previous clinical trial as a precautionary, protocol-specified measure due to detection of serum IgE antibodies or skin-test reactivity to agalsidase beta.

Methods: The rechallenge infusion protocol specified strict patient monitoring conditions and graded dosing and infusion-rate schemes that were adjusted according to each patient's tolerance to the infusion. Six males (age: 26-66 years) were enrolled.

Results: During rechallenge, five patients received between 4 and 27 infusions; one patient voluntarily withdrew after one infusion because of recurrence of infusion-associated reactions. No anaphylactic reactions occurred. All adverse events, including four serious adverse events, were mild or moderate in intensity. Most treatment-related adverse events occurred during infusions (most commonly urticaria, vomiting, nausea, chills, pruritus, hypertension) and were resolved by infusion rate reductions and/or medication. After participation in the study, all patients, including the one who withdrew after one infusion, transitioned to commercial drug.

Conclusions: Agalsidase beta therapy can be successfully reinstated in patients with Fabry disease who have developed IgE antibodies or skin test reactivity to the recombinant enzyme.

Citing Articles

Relevance of Neutralizing Antibodies for the Pharmacokinetics of Pegunigalsidase Alfa in Patients with Fabry Disease.

Lenders M, Menke E, Rudnicki M, Cybulla M, Brand E BioDrugs. 2024; 39(1):153-165.

PMID: 39614966 PMC: 11750932. DOI: 10.1007/s40259-024-00690-1.

Safety and Tolerability of a Shorter Agalsidase Beta Infusion Time in Patients with Classic or Later-Onset Fabry Disease.

Germain D, Porto Vasconcelos A, Tran Thi Phuong L, Bedreddine N, Turcan M, Trang W Biomedicines. 2024; 12(11).

PMID: 39595144 PMC: 11591728. DOI: 10.3390/biomedicines12112578.

Reducing agalsidase beta infusion time in Fabry patients: low incidence of antibody formation and infusion-associated reactions in an Italian multicenter study.

Mignani R, Americo C, Aucella F, Battaglia Y, Cianci V, Sapuppo A Orphanet J Rare Dis. 2024; 19(1):38.

PMID: 38308295 PMC: 10835838. DOI: 10.1186/s13023-024-03049-5.

Brazilian consensus recommendations for the diagnosis, screening, and treatment of individuals with fabry disease: Committee for Rare Diseases - Brazilian Society of Nephrology/2021.

Silva C, Modelli de Andrade L, Vaisbich M, Barreto F J Bras Nefrol. 2022; 44(2):249-267.

PMID: 35212703 PMC: 9269181. DOI: 10.1590/2175-8239-JBN-2021-0208.

Mechanisms of Neutralizing Anti-drug Antibody Formation and Clinical Relevance on Therapeutic Efficacy of Enzyme Replacement Therapies in Fabry Disease.

Lenders M, Brand E Drugs. 2021; 81(17):1969-1981.

PMID: 34748189 PMC: 8602155. DOI: 10.1007/s40265-021-01621-y.