Somatic gene mutations in the motor cortex of patients with sporadic amyotrophic lateral sclerosis.

González-Velasco, Óscar; Voith von Voithenberg, Lena; Forsberg, Karin M E; Decker, Lorena; Yang, Xiaoxu; Yilmaz, Rüstem; Tulasi, Nikshitha; Andersen, Peter M; Parlato, Rosanna; Brenner, David; Freischmidt, Axel; Menge, Sonja; Weishaupt, Jochen H; Brors, Benedikt; Schlachetzki, Johannes C M

doi:10.1093/brain/awaf460

Journal Article

DKFZ-2026-00535

Somatic gene mutations in the motor cortex of patients with sporadic amyotrophic lateral sclerosis.

González-Velasco, Ó. (First author)DKFZ* ; Parlato, R. ; Yilmaz, R. ; Decker, L. ; Menge, S. ; Freischmidt, A. ; Yang, X. ; Tulasi, N. ; Brenner, D. ; Andersen, P. M. ; Forsberg, K. M. E. ; Schlachetzki, J. C. M. ; Brors, B.DKFZ* ; Voith von Voithenberg, L. (Last author)DKFZ* ; Weishaupt, J. H.

2026
Oxford Univ. Press Oxford

Brain 149(3), 778 - 784 (2026) [10.1093/brain/awaf460]

Abstract: Amyotrophic lateral sclerosis (ALS) is characterized by the progressive degeneration of cortical and spinal motor neurons. Mendelian germline mutations often cause familial ALS (fALS) but only approximately 10% of sporadic ALS cases (sALS). We leveraged DNA and single-cell RNA sequencing data from autopsy tissue to explore the presence of somatic mosaic variants in sALS cases. Deep targeted panel sequencing of known ALS disease genes in motor cortex tissue revealed an enrichment of low allele frequency variants in sALS, but not in fALS with an identified monogenic cause. In silico analysis predicted increased pathogenicity of mosaic mutations in various known ALS mutational hot-spots. In particular, we identified the somatic FUS variant p.E516X, located in an established hotspot for germline ALS mutations, which leads to nucleo-cytoplasmic mislocalization and aggregation typical for ALS FUS pathology. Additionally, we performed somatic variant calling on single-cell RNA-sequencing data from sALS tissue and revealed a specific accumulation of somatic variants in excitatory neurons, reinforcing a neuron-autonomous disease initiation. Collectively, this study indicates that somatic mutations within the motor cortex, especially in excitatory neurons, may contribute to sALS development.

Keyword(s): Humans (MeSH) ; Amyotrophic Lateral Sclerosis: genetics (MeSH) ; Amyotrophic Lateral Sclerosis: pathology (MeSH) ; Motor Cortex: metabolism (MeSH) ; Motor Cortex: pathology (MeSH) ; Mutation: genetics (MeSH) ; Female (MeSH) ; Male (MeSH) ; Middle Aged (MeSH) ; Aged (MeSH) ; RNA-Binding Protein FUS: genetics (MeSH) ; amyotrophic lateral sclerosis ; excitatory neurons ; neuronal somatic mosaicism ; somatic variants ; RNA-Binding Protein FUS ; FUS protein, human

Classification:

ddc:610

Note: #EA:B330#LA:B330#

Contributing Institute(s):

Angewandte Bioinformatik (B330)

Research Program(s):

312 - Funktionelle und strukturelle Genomforschung (POF4-312) (POF4-312)

Appears in the scientific report 2026

Database coverage:
Medline

; BIOSIS Previews ; Biological Abstracts ; Clarivate Analytics Master Journal List ; Current Contents - Clinical Medicine ; Current Contents - Life Sciences ; Ebsco Academic Search ; Essential Science Indicators ; IF >= 10 ; JCR ; Nationallizenz

; SCOPUS ; Science Citation Index Expanded ; Web of Science Core Collection

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Record created 2026-03-09, last modified 2026-03-19

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