AI Article Synopsis

  • Gene addition and editing therapies for β-thalassemia, particularly betibeglogene autotemcel (beti-cel), show promise as potentially curative options, with real-world studies demonstrating their effectiveness and safety.* -
  • Out of 15 patients evaluated for treatment with beti-cel, 8 were treated post-busulfan conditioning, achieving transfusion independence within 8 to 59 days, while experiencing some acute toxicity typical of the conditioning regimen.* -
  • Monitoring of patients revealed several unexpected side effects, including endocrine dysfunction, posttreatment depression and anxiety in one patient, and fatigue impacting quality of life in another, underscoring the need for careful management of these complications.*

Article Abstract

Gene addition and editing strategies for transfusion-dependent β-thalassemia have gained momentum as potentially curative treatment options, with studies showcasing their efficacy and safety. We report, to our knowledge, the first real-world application of betibeglogene autotemcel (beti-cel; Zynteglo) during its period of active license in Europe from January 2020 to March 2022 for patients aged ≥12 years without a β0/β0 genotype and without a HLA-matched sibling donor, before beti-cel marketing authorization was withdrawn by its holder because of nonsafety reasons. Among 15 screened patients, 4 opted out for fertility and safety concerns, 2 were excluded because of marked hepatic siderosis, and 1 had apheresis collection failure. Eight patients received beti-cel after busulfan myeloablative conditioning, all achieving transfusion independence within 8 to 59 days, with posttreatment hemoglobin levels ranging from 11.3 to 19.3 g/dL. No deaths occurred, but acute toxicity mirrored busulfan's known effects. Posttreatment platelet management faced challenges because of HLA-antibodies in 3 patients. Monitoring up to month 24 revealed pituitary-gonadal endocrine dysfunction in all 3 female and in 2 of 5 male patients. Additionally, we observed unexpected posttreatment sequelae: 1 patient developed polycythemia that could not be explained by known genetic or acquired mechanisms, 1 patient developed posttreatment depression and anxiety prohibiting her from returning to work, and 1 patient developed fatigue severely compromising both quality of life and work capacity. This real-world experience corroborates beti-cel's efficacy and safety and provides information on adverse events observed during real-world use of the therapy.

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http://dx.doi.org/10.1182/bloodadvances.2024014104DOI Listing

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