Genetic epidemiology of amyotrophic lateral sclerosis in Norway - a 2-year population based study

dc.date.accessioned	2022-08-17T15:48:45Z
dc.date.available	2022-08-17T15:48:45Z
dc.date.created	2022-05-20T12:31:28Z
dc.date.issued	2022
dc.identifier.citation	Olsen, Cathrine Goberg Busk, Øyvind Løvold Aanjesen, Tori Navestad Alstadhaug, Karl Bjørnar Bjørnå, Ingrid Kristine Braathen, Geir Julius Breivik, Kristin Lif Demic, Natasha Flemmen, Heidi Øyen Hallerstig, Erika HogenEsch, Ineke Holla, Øystein Lunde Jøntvedt, Anne Berit Kampman, Margitta T. Kleveland, Grethe Kvernmo, Helene Ballo Ljøstad, Unn Maniaol, Angelina Morsund, Åse Hagen Nakken, Ola Novy, Camilla Rekand, Tiina Schlüter, Katrin Ruth Schuler, Stephan Tveten, Kristian Tysnes, Ole-Bjørn Holmøy, Trygve Høyer, Helle . Genetic epidemiology of amyotrophic lateral sclerosis in Norway - a 2-year population based study. Neuroepidemiology. 2022, 1-22
dc.identifier.uri	http://hdl.handle.net/10852/95034
dc.description.abstract	Background: Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease that affects motor neurons. In Europe, disease-causing genetic variants have been identified in 40-70% of familial ALS patients and approximately in 5% of sporadic ALS patients. In Norway, the contribution of genetic variants to ALS has not yet been studied. In light of the potential development of personalized medicine, knowledge of genetic causes of ALS in a population is becoming increasingly important. The present study provides clinical and genetic data on familial and sporadic ALS patients in a Norwegian population-based cohort. Methods: Blood samples and clinical information from ALS patients were obtained at all 17 neurological departments throughout Norway during a 2-year period. Genetic analysis of the samples involved expansion analysis of C9orf72 and exome sequencing targeting 30 known ALS-linked genes. The variants were classified using genotype-phenotype correlations and bioinformatics tools. Results: A total of 279 ALS patients were included in the study. Of these, 11.5% had one or several family members affected with ALS, whereas 88.5% had no known family history of ALS. A genetic cause of ALS was identified in 31 individuals (11.1%), among which 18 (58.1%) were familial and 13 (41.9%) were sporadic. The most common genetic cause was the C9orf72 expansion (6.8%), which was identified in 8 familial and 11 sporadic ALS patients. Pathogenic or likely pathogenic variants of SOD1 and TBK1 were identified in 10 familial and 2 sporadic cases. C9orf72 expansions dominated in patients from the Northern and Central regions, whereas SOD1 variants dominated in patients from the South-Eastern region. Conclusion: In the present study, we identified several pathogenic gene variants in both familial and sporadic ALS patients. Restricting genetic analysis to only familial cases would miss more than 40 percent of those with a disease-causing genetic variant, indicating the need for genetic analysis in sporadic cases as well.
dc.description.abstract	Genetic epidemiology of amyotrophic lateral sclerosis in Norway - a 2-year population based study
dc.language	EN
dc.publisher	Karger
dc.rights	Attribution-NonCommercial 4.0 International
dc.rights.uri	https://creativecommons.org/licenses/by-nc/4.0/
dc.title	Genetic epidemiology of amyotrophic lateral sclerosis in Norway - a 2-year population based study
dc.title.alternative	ENEngelskEnglishGenetic epidemiology of amyotrophic lateral sclerosis in Norway - a 2-year population based study
dc.type	Journal article
dc.creator.author	Olsen, Cathrine Goberg
dc.creator.author	Busk, Øyvind Løvold
dc.creator.author	Aanjesen, Tori Navestad
dc.creator.author	Alstadhaug, Karl Bjørnar
dc.creator.author	Bjørnå, Ingrid Kristine
dc.creator.author	Braathen, Geir Julius
dc.creator.author	Breivik, Kristin Lif
dc.creator.author	Demic, Natasha
dc.creator.author	Flemmen, Heidi Øyen
dc.creator.author	Hallerstig, Erika
dc.creator.author	HogenEsch, Ineke
dc.creator.author	Holla, Øystein Lunde
dc.creator.author	Jøntvedt, Anne Berit
dc.creator.author	Kampman, Margitta T.
dc.creator.author	Kleveland, Grethe
dc.creator.author	Kvernmo, Helene Ballo
dc.creator.author	Ljøstad, Unn
dc.creator.author	Maniaol, Angelina
dc.creator.author	Morsund, Åse Hagen
dc.creator.author	Nakken, Ola
dc.creator.author	Novy, Camilla
dc.creator.author	Rekand, Tiina
dc.creator.author	Schlüter, Katrin Ruth
dc.creator.author	Schuler, Stephan
dc.creator.author	Tveten, Kristian
dc.creator.author	Tysnes, Ole-Bjørn
dc.creator.author	Holmøy, Trygve
dc.creator.author	Høyer, Helle
cristin.unitcode	185,53,0,0
cristin.unitname	Institutt for klinisk medisin
cristin.ispublished	true
cristin.fulltext	original
cristin.qualitycode	1
dc.identifier.cristin	2025960
dc.identifier.bibliographiccitation	info:ofi/fmt:kev:mtx:ctx&ctx_ver=Z39.88-2004&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.jtitle=Neuroepidemiology&rft.volume=&rft.spage=1&rft.date=2022
dc.identifier.jtitle	Neuroepidemiology
dc.identifier.startpage	1
dc.identifier.endpage	22
dc.identifier.doi	https://doi.org/10.1159/000525091
dc.identifier.urn	URN:NBN:no-97544
dc.type.document	Tidsskriftartikkel
dc.type.peerreviewed	Peer reviewed
dc.source.issn	0251-5350
dc.identifier.fulltext	Fulltext https://www.duo.uio.no/bitstream/handle/10852/95034/1/525091.pdf
dc.type.version	PublishedVersion
dc.relation.project	HSØ/2021097
dc.relation.project	STHF/8208.03 + 8208.04
dc.relation.project	ALSNORGE/8208.05