Acid sphingomyelinase deficiency in France: a retrospective survival study-Reference-Cited by-同舟云学术

Acid sphingomyelinase deficiency in France: a retrospective survival study

Published:2024-08-05 Issue:1 Volume:19 Page:
ISSN:1750-1172
Container-title:Orphanet Journal of Rare Diseases
language:en
Short-container-title:Orphanet J Rare Dis

Author:

Mauhin Wladimir,Guffon Nathalie,Vanier Marie T.,Froissart Roseline,Cano Aline,Douillard Claire,Lavigne Christian,Héron Bénédicte,Belmatoug Nadia,Uzunhan Yurdagül,Lacombe Didier,Levade Thierry,Duvivier Aymeric,Pulikottil-Jacob Ruth,Laredo Fernando,Pichard Samia,Lidove Olivier^ORCID, ,Abi-Wardé Marie-Thérèse,Berger Marc,Berthoux Emilie,Cabannes-Hamy Aurélie,Camou Fabrice,Cathebras Pascal,Grobost Vincent,Keraen Jérémy,Kuster Alice,Lioger Bertrand,Mehdaoui Anas,Merlot Claire,Michaud Martin,Reynaud-Gaubert Martine-Louise,Schlemmer Fréderic,Servettaz Amélie,Stavris Chloé,Trouillier Sébastien

Abstract

Abstract Background Acid sphingomyelinase deficiency (ASMD) or Niemann–Pick disease types A, A/B, and B is a progressive, life-limiting, autosomal recessive disorder caused by sphingomyelin phosphodiesterase 1 (SMPD1) gene mutations. There is a need to increase the understanding of morbidity and mortality across children to adults diagnosed with ASMD. Methods This observational retrospective survey analysed medical records of patients with ASMD with retrievable data from 27 hospitals in France, diagnosed/followed up between 1st January 1990 and 31st December 2020. Eligible records were abstracted to collect demographic, medical/developmental history, and mortality data. Survival outcomes were estimated from birth until death using Kaplan–Meier survival analyses; standardised mortality ratio (SMR) was also explored. Results A total of 118 medical records of patients with ASMD (type B [n = 94], type A [n = 15], and type A/B [n = 9]) were assessed. The majority of patients were males (63.6%); the median [range] age at diagnosis was 8.0 [1.0–18.0] months (type A), 1.0 [0–3] year (type A/B), and 5.5 [0–73] years (type B). Overall, 30 patients were deceased at the study completion date; the median [range] age at death for patients with ASMD type A (n = 14) was 1 [0–3.6] year, type A/B (n = 6) was 8.5 [3.0–30.9] years, and type B (n = 10) was 57.6 [3.4–74.1] years. The median [95% confidence interval (CI)] survival age from birth in patients with ASMD type A and type A/B was 2.0 [1.8–2.7] years and 11.4 [5.5–18.5] years, respectively. Survival analysis in ASMD type B was explored using SMR [95% CI] analysis (3.5 [1.6–5.9]), which showed that age-specific deaths in the ASMD type B population were 3.5 times more frequent than those in the general French population. The causes of death were mostly severe progressive neurodegeneration (type A: 16.7%), cancer (type B: 16.7%), or unspecified (across groups: 33.3%). Conclusions This study illustrated a substantial burden of illness with high mortality rates in patients with ASMD, including adults with ASMD type B, in France.

Funder

Sanofi

Publisher

Springer Science and Business Media LLC

Link

https://link.springer.com/content/pdf/10.1186/s13023-024-03234-6.pdf

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