TY - JOUR
T1 - The phenotypic spectrum and genetic determinants of severe spinal muscular atrophy in individuals with a single SMN2 copy
T2 - an international retrospective observational study
AU - Cicala, Gianpaolo
AU - Capasso, Anna
AU - Villa, Marianna
AU - Coratti, Giorgia
AU - Arpaia, Chiara
AU - Agosto, Caterina
AU - Corti, Stefania
AU - Ricci, Federica
AU - Bruno, Claudio
AU - Matesanz, Susan
AU - Gross, Brianna
AU - Mendoza, Daniel Guillen
AU - Kuntz, Nancy
AU - Kirschner, Janbernd
AU - Ziegler, Andreas
AU - Servais, Laurent
AU - Asselman, Fay Linn
AU - van der Pol, Ludo
AU - Castiglioni, Claudia
AU - Nascimiento, Andres
AU - Tizzano, Eduardo Fidel
AU - Mendonça, Rodrigo Holanda
AU - Zanoteli, Edmar
AU - Munot, Pinki
AU - Scoto, Mariacristina
AU - Finkel, Richard
AU - Pane, Marika
AU - Tiziano, Francesco Danilo
AU - Mercuri, Eugenio
N1 - Publisher Copyright:
© 2026 The Author(s). Published by Elsevier Ltd. This is an open access article under the CC BY-NC-ND license. http://creativecommons.org/licenses/by-nc-nd/4.0/
PY - 2026/5
Y1 - 2026/5
N2 - Background: Spinal Muscular Atrophy (SMA) is a phenotypically heterogenous disease. The Survival Motor Neuron 2 (SMN2) gene copy number can partially predict the clinical severity of SMA, with a single SMN2 copy generally associated with the most severe phenotypes. The aim of this retrospective observational study was to explore the spectrum of phenotypes associated with one SMN2 copy and the possible association with genotype and outcome. Methods: We conducted a retrospective observational study of individuals with genetically confirmed SMA (biallelic Survival Motor Neuron 1 [SMN1] variants) and one SMN2 copy, recruited from 36 Italian neuromuscular centres and additional 28 centres from nine other countries (Austria, Belgium, Brazil, Chile, Germany, Netherlands, Spain, United Kingdom and United States) between January 2015 and November 2025.Individuals were included irrespective of age or phenotype; those with incomplete genetic data or confounding diagnoses were excluded. The primary outcome was the phenotypic spectrum associated with a single SMN2 copy, including clinical severity, genotype, treatment exposure, and survival at last follow-up. Findings: Sixty-five individuals with one SMN2 copy were included. Neonatal onset was observed in 50/65 (77%). The predominant phenotype was type 0 (39/50, 78%), followed by type 1.1 (6/50, 12%). Five individuals with neonatal onset had prenatal signs (reduced foetal movements and cardiac malformation), but no contractures reported. All individuals with neonatal onset had homozygous deletions of SMN1. The remaining 15/65 (23%) had later onset, with milder phenotypes and all but two presented either with an heterozygous SMN1 deletion associated with a point mutation, or with c.859G>C(p.Gly287Arg) variant in SMN2. Interpretation: Our findings confirm that type 0 is the most frequent phenotype associated with one SMN2 copy, but the boundaries between neonatal-onset phenotypes appear to be fluid. The individuals with one SMN2 copy with milder phenotypes carried variants known to mitigate disease severity. Further prospective studies are needed to better define genotype–phenotype correlations and inform treatment decisions in this population. Funding: Some of the data in this study originate from disease registries at least partially funded by Biogen, Novartis and Roche.
AB - Background: Spinal Muscular Atrophy (SMA) is a phenotypically heterogenous disease. The Survival Motor Neuron 2 (SMN2) gene copy number can partially predict the clinical severity of SMA, with a single SMN2 copy generally associated with the most severe phenotypes. The aim of this retrospective observational study was to explore the spectrum of phenotypes associated with one SMN2 copy and the possible association with genotype and outcome. Methods: We conducted a retrospective observational study of individuals with genetically confirmed SMA (biallelic Survival Motor Neuron 1 [SMN1] variants) and one SMN2 copy, recruited from 36 Italian neuromuscular centres and additional 28 centres from nine other countries (Austria, Belgium, Brazil, Chile, Germany, Netherlands, Spain, United Kingdom and United States) between January 2015 and November 2025.Individuals were included irrespective of age or phenotype; those with incomplete genetic data or confounding diagnoses were excluded. The primary outcome was the phenotypic spectrum associated with a single SMN2 copy, including clinical severity, genotype, treatment exposure, and survival at last follow-up. Findings: Sixty-five individuals with one SMN2 copy were included. Neonatal onset was observed in 50/65 (77%). The predominant phenotype was type 0 (39/50, 78%), followed by type 1.1 (6/50, 12%). Five individuals with neonatal onset had prenatal signs (reduced foetal movements and cardiac malformation), but no contractures reported. All individuals with neonatal onset had homozygous deletions of SMN1. The remaining 15/65 (23%) had later onset, with milder phenotypes and all but two presented either with an heterozygous SMN1 deletion associated with a point mutation, or with c.859G>C(p.Gly287Arg) variant in SMN2. Interpretation: Our findings confirm that type 0 is the most frequent phenotype associated with one SMN2 copy, but the boundaries between neonatal-onset phenotypes appear to be fluid. The individuals with one SMN2 copy with milder phenotypes carried variants known to mitigate disease severity. Further prospective studies are needed to better define genotype–phenotype correlations and inform treatment decisions in this population. Funding: Some of the data in this study originate from disease registries at least partially funded by Biogen, Novartis and Roche.
KW - OneSMN2copy
KW - Prenatal SMA
KW - Spinal muscular atrophy
KW - Type 0 SMA
UR - https://www.scopus.com/pages/publications/105037942249
U2 - 10.1016/j.eclinm.2026.103931
DO - 10.1016/j.eclinm.2026.103931
M3 - Article
AN - SCOPUS:105037942249
SN - 2589-5370
VL - 95
JO - EClinicalMedicine
JF - EClinicalMedicine
M1 - 103931
ER -