Observation of the natural course of type 3 spinal muscular atrophy: data from the polish registry of spinal muscular atrophy

Anna Lusakowska; Maria Jedrzejowska; Anna Kaminska; Katarzyna Janiszewska; Przemysław Grochowski; Janusz Zimowski; Janusz Sierdzinski; Anna Kostera-Pruszczyk

doi:10.1186/s13023-021-01771-y

Orphanet Journal of Rare Diseases (Mar 2021)

Observation of the natural course of type 3 spinal muscular atrophy: data from the polish registry of spinal muscular atrophy

Anna Lusakowska,
Maria Jedrzejowska,
Anna Kaminska,
Katarzyna Janiszewska,
Przemysław Grochowski,
Janusz Zimowski,
Janusz Sierdzinski,
Anna Kostera-Pruszczyk

Affiliations

Anna Lusakowska: Department of Neurology, European Reference Network EURO-NMD, Medical University of Warsaw
Maria Jedrzejowska: Rare Diseases Research Platform, Mossakowski Medical Research Institute, Polish Academy of Sciences
Anna Kaminska: Department of Neurology, European Reference Network EURO-NMD, Medical University of Warsaw
Katarzyna Janiszewska: Department of Neurology, European Reference Network EURO-NMD, Medical University of Warsaw
Przemysław Grochowski: Student Research Group of Department of Neurology, Medical University of Warsaw
Janusz Zimowski: Department of Genetics, Institute of Psychiatry and Neurology
Janusz Sierdzinski: Department of Medical Informatics and Telemedicine, Medical University of Warsaw
Anna Kostera-Pruszczyk: Department of Neurology, European Reference Network EURO-NMD, Medical University of Warsaw

DOI: https://doi.org/10.1186/s13023-021-01771-y
Journal volume & issue: Vol. 16, no. 1
pp. 1 – 9

Abstract

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Abstract Background Spinal muscular atrophy (SMA) is one of the most frequent and severe genetic diseases leading to premature death or severe motor disability. New therapies have been developed in recent years that change the natural history of the disease. The aim of this study is to describe patients included in the Polish Registry of SMA, with a focus on the course of type 3 SMA (SMA3) before the availability of disease-modifying treatments. Results 790 patients with SMA were included in the registry (173 with type 1 [SMA1], 218 with type 2 [SMA2], 393 with SMA3, and six with type 4 SMA [SMA4]), most (52%) of whom were adults. Data on SMN2 gene copy number were available for 672 (85%) patients. The mean age of onset was 5 months for SMA1, 11.5 months for SMA2, and 4.5 years for SMA3. In patients with SMA3, the first symptoms occurred earlier in those with three copies of SMN2 than in those with four copies of SMN2 (3.2 years vs. 6.7 years). The age of onset of SMA3 was younger in girls than in boys (3.1 years vs. 5.7 years), with no new cases observed in women older than 16 years. Male patients outnumbered female patients, especially among patients with SMA3b (49 female vs. 85 male patients) and among patients with SMA3 with four copies of SMN2 (30 female vs. 69 male patients). 44% of patients with SMA3 were still able to walk; in those who were not still able to walk, the mean age of immobilization was 14.0 years. Patients with SMA3a (age of onset < 3 years) and three copies of SMN2 had significantly worse prognosis for remaining ambulant than patients with SMA3b (age of onset ≥ 3 years) and four copies of SMN2. Conclusions The Registry of SMA is an effective tool for assessing the disease course in the real world setting. SMN2 copy number is an important prognostic factor for the age of onset and ambulation in SMA3. Sex and age of disease onset also strongly affect the course of SMA. Data supplied by this study can aid treatment decisions.

Published in Orphanet Journal of Rare Diseases

ISSN: 1750-1172 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://ojrd.biomedcentral.com

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