Family-based exome sequencing identifies RBM45 as a possible candidate gene for frontotemporal dementia and amyotrophic lateral sclerosis

Julie van der Zee; Lubina Dillen; Yalda Baradaran-Heravi; Helena Gossye; Cemile Koçoğlu; Ivy Cuyt; Bart Dermaut; Anne Sieben; Jonathan Baets; Peter De Jonghe; Rik Vandenberghe; Peter De Deyn; Patrick Cras; Sebastiaan Engelborghs; Christine Van Broeckhoven; BELNEU Consortium

doi:10.1016/j.nbd.2021.105421

Family-based exome sequencing identifies RBM45 as a possible candidate gene for frontotemporal dementia and amyotrophic lateral sclerosis

Neurobiol Dis. 2021 Aug:156:105421. doi: 10.1016/j.nbd.2021.105421. Epub 2021 Jun 9.

Authors

Affiliations

¹ Neurodegenerative Brain Diseases, VIB Center for Molecular Neurology, VIB, Antwerp, Belgium; Institute Born-Bunge, Antwerp, Belgium. Electronic address: julie.vanderzee@uantwerpen.vib.be.
² Neurodegenerative Brain Diseases, VIB Center for Molecular Neurology, VIB, Antwerp, Belgium; Institute Born-Bunge, Antwerp, Belgium.
³ Neurodegenerative Brain Diseases, VIB Center for Molecular Neurology, VIB, Antwerp, Belgium; Institute Born-Bunge, Antwerp, Belgium; Department of Neurology, Antwerp University Hospital, Antwerp, Belgium; Department of Neurology and Memory Clinic, Hospital Network Antwerp (ZNA), Middelheim and Hoge Beuken, Antwerp, Belgium.
⁴ Center for Medical Genetics, Ghent University Hospital, Ghent, Belgium; Department of Biomolecular Medicine, Faculty of Medicine and Health Sciences, Ghent University, Ghent, Belgium.
⁵ Institute Born-Bunge, Antwerp, Belgium; Department of Neurology, Ghent University Hospital, Ghent, Belgium.
⁶ Institute Born-Bunge, Antwerp, Belgium; Department of Neurology, Antwerp University Hospital, Antwerp, Belgium; Translational Neurosciences, Faculty of Medicine and Health Sciences, UAntwerpen, Antwerp, Belgium.
⁷ Institute Born-Bunge, Antwerp, Belgium; Department of Neurology, Antwerp University Hospital, Antwerp, Belgium.
⁸ Department of Neurology University Hospitals and Department of Neurosciences, KU Leuven, Leuven, Belgium.
⁹ Institute Born-Bunge, Antwerp, Belgium; Department of Neurology and Memory Clinic, Hospital Network Antwerp (ZNA), Middelheim and Hoge Beuken, Antwerp, Belgium; Department of Neurology and Alzheimer Center Groningen, University Medical Center Groningen (UMCG), Groningen, The Netherlands.
¹⁰ Institute Born-Bunge, Antwerp, Belgium; Department of Neurology and Center for Neurosciences, UZ Brussel and Vrije Universiteit Brussel, Brussels, Belgium.
¹¹ Neurodegenerative Brain Diseases, VIB Center for Molecular Neurology, VIB, Antwerp, Belgium; Institute Born-Bunge, Antwerp, Belgium. Electronic address: christine.vanbroeckhoven@uantwerpen.vib.be.

PMID: 34118419
DOI: 10.1016/j.nbd.2021.105421

Abstract

Neurodegenerative disorders like frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS) are pathologically characterized by toxic protein deposition in the cytoplasm or nucleus of affected neurons and glial cells. Many of these aggregated proteins belong to the class of RNA binding proteins (RBP), and, when mutated, account for a significant subset of familial ALS and FTD cases. Here, we present first genetic evidence for the RBP gene RBM45 in the FTD-ALS spectrum. RBM45 shows many parallels with other FTD-ALS associated genes and proteins. Multiple lines of evidence have demonstrated that RBM45 is an RBP that, upon mutation, redistributes to the cytoplasm where it co-aggregates with other RBPs into cytoplasmic stress granules (SG), evolving to persistent toxic TDP-43 immunoreactive inclusions. Exome sequencing in two affected first cousins of a heavily affected early-onset dementia family listed a number of candidate genes. The gene with the highest pathogenicity score was the RBP gene RBM45. In the family, the RBM45 Arg183* nonsense mutation co-segregated in both affected cousins. Validation in an unrelated patient (n = 548) / control (n = 734) cohort identified an additional RBM45 Arg183* carrier with bvFTD on a shared 4 Mb haplotype. Transcript and protein expression analysis demonstrated loss of nuclear RBM45, suggestive of a loss-of-function disease mechanism. Further, two more ultra-rare VUS, one in the nuclear localization signal (NLS, p.Lys456Arg) in an ALS patient and one in the intrinsically disordered homo-oligomer assembly (HOA) domain (p.Arg314Gln) in a patient with nfvPPA were detected. Our findings suggest that the pathomechanisms linking RBM45 with FTD and ALS may be related to its loss of nuclear function as a mediator of mRNA splicing, cytoplasmic retention or its inability to form homo-oligomers, leading to aggregate formation with trapping of other RBPs including TDP-43, which may accumulate into persisted TDP-43 inclusions.

Keywords: Amyotrophic lateral sclerosis, ALS; Exome sequencing; Frontotemporal dementia, FTD; Neurodegeneration; RBM45; RNA binding protein; TDP-43 proteinopathy.

Publication types

Multicenter Study
Research Support, Non-U.S. Gov't

MeSH terms

Aged
Aged, 80 and over
Amino Acid Sequence
Amyotrophic Lateral Sclerosis / diagnosis
Amyotrophic Lateral Sclerosis / epidemiology
Amyotrophic Lateral Sclerosis / genetics*
Belgium / epidemiology
Cohort Studies
Exome Sequencing / methods*
Female
Frontotemporal Dementia / diagnosis
Frontotemporal Dementia / epidemiology
Frontotemporal Dementia / genetics*
Genetic Association Studies / methods*
Humans
Male
Middle Aged
Nerve Tissue Proteins / genetics*
Pedigree
RNA-Binding Proteins / genetics*

Substances

Nerve Tissue Proteins
RBM45 protein, human
RNA-Binding Proteins