Clinical and genetic features of amyotrophic lateral sclerosis patients with C9orf72 mutations

Maximilian Wiesenfarth; Kornelia Günther; Kathrin Müller; Simon Witzel; Ulrike Weiland; Kristina Mayer; Christine Herrmann; David Brenner; Joachim Schuster; Axel Freischmidt; Dorothée Lulé; Thomas Meyer; Martin Regensburger; Torsten Grehl; Alexander Emmer; Susanne Petri; Julian Großkreutz; Annekathrin Rödiger; Robert Steinbach; Thomas Klopstock; Peter Reilich; Florian Schöberl; Joachim Wolf; Tim Hagenacker; Ute Weyen; Daniel Zeller; Albert C Ludolph; Johannes Dorst

doi:10.1093/braincomms/fcad087

Clinical and genetic features of amyotrophic lateral sclerosis patients with C9orf72 mutations

Brain Commun. 2023 Mar 21;5(2):fcad087. doi: 10.1093/braincomms/fcad087. eCollection 2023.

Authors

Maximilian Wiesenfarth¹, Kornelia Günther¹, Kathrin Müller¹, Simon Witzel¹, Ulrike Weiland¹, Kristina Mayer¹, Christine Herrmann¹, David Brenner¹, Joachim Schuster¹, Axel Freischmidt¹, Dorothée Lulé¹, Thomas Meyer², Martin Regensburger³, Torsten Grehl⁴, Alexander Emmer⁵, Susanne Petri⁶, Julian Großkreutz⁷, Annekathrin Rödiger⁸, Robert Steinbach⁸, Thomas Klopstock^{9

10

11}, Peter Reilich⁹, Florian Schöberl⁹, Joachim Wolf¹², Tim Hagenacker¹³, Ute Weyen¹⁴, Daniel Zeller¹⁵, Albert C Ludolph^{1

16}, Johannes Dorst¹

Affiliations

¹ Department of Neurology, Ulm University, 89081 Ulm, Germany.
² Department of Neurology, Center for ALS and other Motor Neuron Disorders, Charité-Universitätsmedizin Berlin, Corporate Member of Freie Universität Berlin, Humboldt-Universität zu Berlin, and Berlin Institute of Health, 13353 Berlin, Germany.
³ Department of Molecular Neurology, Friedrich-Alexander-Universität Erlangen-Nürnberg (FAU), 91054 Erlangen, Germany.
⁴ Alfried Krupp Hospital, Rüttenscheid, 45131 Essen, Germany.
⁵ Department of Neurology, Halle University Hospital, 06120 Halle, Germany.
⁶ Department of Neurology, Hannover Medical School, 30625 Hannover, Germany.
⁷ Precision Neurology, University of Lübeck, 23538 Lübeck, Germany.
⁸ Department of Neurology, Jena University Hospital, 07745 Jena, Germany.
⁹ Department of Neurology with Friedrich-Baur-Institute, University Hospital of Ludwig-Maximilians-University, 80336 München, Germany.
¹⁰ German Centre for Neurodegenerative Diseases (DZNE) Site Munich, 81377 Munich, Germany.
¹¹ Munich Cluster for Systems Neurology (SyNergy), 81377 Munich, Germany.
¹² Department of Neurology, Diakonissen Hospital, 68163 Mannheim, Germany.
¹³ Department of Neurology and Center for Translational Neuro and Behavioral Sciences (C-TNBS), University Hospital Essen, 45127 Essen, Germany.
¹⁴ Department of Neurology, Ruhr-University Bochum, BG-Kliniken Bergmannsheil, 44789 Bochum, Germany.
¹⁵ Department of Neurology, University of Würzburg, 97080 Würzburg, Germany.
¹⁶ German Centre for Neurodegenerative Diseases (DZNE) Site Ulm, 89081 Ulm, Germany.

Abstract

An expansion of the GGGGCC hexanucleotide in the non-coding region of C9orf72 represents the most common cause of familial amyotrophic lateral sclerosis. The objective was to describe and analyse the clinical and genetic features of amyotrophic lateral sclerosis patients with C9orf72 mutations in a large population. Between November 2011 and December 2020, clinical and genetic characteristics of n = 248 patients with amyotrophic lateral sclerosis carrying C9orf72 mutations were collected from the clinical and scientific network of German motoneuron disease centres. Clinical parameters included age of onset, diagnostic delay, family history, neuropsychological examination, progression rate, phosphorylated neurofilament heavy chain levels in CSF and survival. The number of repeats was correlated with the clinical phenotype. The clinical phenotype was compared to n = 84 patients with SOD1 mutations and n = 2178 sporadic patients without any known disease-related mutations. Patients with C9orf72 featured an almost balanced sex ratio with 48.4% (n = 120) women and 51.6% (n = 128) men. The rate of 33.9% patients (n = 63) with bulbar onset was significantly higher compared to sporadic (23.4%, P = 0.002) and SOD1 patients (3.1%, P < 0.001). Of note, 56.3% (n = 138) of C9orf72, but only 16.1% of SOD1 patients reported a negative family history (P < 0.001). The GGGGCC hexanucleotide repeat length did not influence the clinical phenotypes. Age of onset (58.0, interquartile range 52.0-63.8) was later compared to SOD1 (50.0, interquartile range 41.0-58.0; P < 0.001), but earlier compared to sporadic patients (61.0, interquartile range 52.0-69.0; P = 0.01). Median survival was shorter (38.0 months) compared to SOD1 (198.0 months, hazard ratio 1.97, 95% confidence interval 1.34-2.88; P < 0.001) and sporadic patients (76.0 months, hazard ratio 2.34, 95% confidence interval 1.64-3.34; P < 0.001). Phosphorylated neurofilament heavy chain levels in CSF (2880, interquartile range 1632-4638 pg/ml) were higher compared to sporadic patients (1382, interquartile range 458-2839 pg/ml; P < 0.001). In neuropsychological screening, C9orf72 patients displayed abnormal results in memory, verbal fluency and executive functions, showing generally worse performances compared to SOD1 and sporadic patients and a higher share with suspected frontotemporal dementia. In summary, clinical features of patients with C9orf72 mutations differ significantly from SOD1 and sporadic patients. Specifically, they feature a more frequent bulbar onset, a higher share of female patients and shorter survival. Interestingly, we found a high proportion of patients with negative family history and no evidence of a relationship between repeat lengths and disease severity.

Keywords: motor neuron disease.