Unknown

Dataset Information

0

Hot-spot KIF5A mutations cause familial ALS.


ABSTRACT: Heterozygous missense mutations in the N-terminal motor or coiled-coil domains of the kinesin family member 5A (KIF5A) gene cause monogenic spastic paraplegia (HSP10) and Charcot-Marie-Tooth disease type 2 (CMT2). Moreover, heterozygous de novo frame-shift mutations in the C-terminal domain of KIF5A are associated with neonatal intractable myoclonus, a neurodevelopmental syndrome. These findings, together with the observation that many of the disease genes associated with amyotrophic lateral sclerosis disrupt cytoskeletal function and intracellular transport, led us to hypothesize that mutations in KIF5A are also a cause of amyotrophic lateral sclerosis. Using whole exome sequencing followed by rare variant analysis of 426 patients with familial amyotrophic lateral sclerosis and 6137 control subjects, we detected an enrichment of KIF5A splice-site mutations in amyotrophic lateral sclerosis (2/426 compared to 0/6137 in controls; P = 4.2 × 10-3), both located in a hot-spot in the C-terminus of the protein and predicted to affect splicing exon 27. We additionally show co-segregation with amyotrophic lateral sclerosis of two canonical splice-site mutations in two families. Investigation of lymphoblast cell lines from patients with KIF5A splice-site mutations revealed the loss of mutant RNA expression and suggested haploinsufficiency as the most probable underlying molecular mechanism. Furthermore, mRNA sequencing of a rare non-synonymous missense mutation (predicting p.Arg1007Gly) located in the C-terminus of the protein shortly upstream of the splice donor of exon 27 revealed defective KIF5A pre-mRNA splicing in respective patient-derived cell lines owing to abrogation of the donor site. Finally, the non-synonymous single nucleotide variant rs113247976 (minor allele frequency = 1.00% in controls, n = 6137), also located in the C-terminal region [p.(Pro986Leu) in exon 26], was significantly enriched in familial amyotrophic lateral sclerosis patients (minor allele frequency = 3.40%; P = 1.28 × 10-7). Our study demonstrates that mutations located specifically in a C-terminal hotspot of KIF5A can cause a classical amyotrophic lateral sclerosis phenotype, and underline the involvement of intracellular transport processes in amyotrophic lateral sclerosis pathogenesis.

SUBMITTER: Brenner D 

PROVIDER: S-EPMC5837483 | biostudies-literature | 2018 Mar

REPOSITORIES: biostudies-literature

altmetric image

Publications

Hot-spot KIF5A mutations cause familial ALS.

Brenner David D   Yilmaz Rüstem R   Müller Kathrin K   Grehl Torsten T   Petri Susanne S   Meyer Thomas T   Grosskreutz Julian J   Weydt Patrick P   Ruf Wolfgang W   Neuwirth Christoph C   Weber Markus M   Pinto Susana S   Claeys Kristl G KG   Schrank Berthold B   Jordan Berit B   Knehr Antje A   Günther Kornelia K   Hübers Annemarie A   Zeller Daniel D   Kubisch Christian C   Jablonka Sibylle S   Sendtner Michael M   Klopstock Thomas T   de Carvalho Mamede M   Sperfeld Anne A   Borck Guntram G   Volk Alexander E AE   Dorst Johannes J   Weis Joachim J   Otto Markus M   Schuster Joachim J   Del Tredici Kelly K   Braak Heiko H   Danzer Karin M KM   Freischmidt Axel A   Meitinger Thomas T   Strom Tim M TM   Ludolph Albert C AC   Andersen Peter M PM   Weishaupt Jochen H JH  

Brain : a journal of neurology 20180301 3


Heterozygous missense mutations in the N-terminal motor or coiled-coil domains of the kinesin family member 5A (KIF5A) gene cause monogenic spastic paraplegia (HSP10) and Charcot-Marie-Tooth disease type 2 (CMT2). Moreover, heterozygous de novo frame-shift mutations in the C-terminal domain of KIF5A are associated with neonatal intractable myoclonus, a neurodevelopmental syndrome. These findings, together with the observation that many of the disease genes associated with amyotrophic lateral scl  ...[more]

Similar Datasets

| S-EPMC3032425 | biostudies-literature
2022-02-17 | GSE196539 | GEO
2021-09-01 | GSE173364 | GEO
| S-EPMC5042851 | biostudies-literature
| S-EPMC3812167 | biostudies-literature
| S-EPMC7140863 | biostudies-literature
2022-02-17 | GSE196537 | GEO
2022-02-17 | GSE196538 | GEO
2022-06-09 | PXD031012 | Pride
| S-EPMC5867896 | biostudies-other