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Literature DB >> 29033165

Molecular epidemiological study of familial amyotrophic lateral sclerosis in Japanese population by whole-exome sequencing and identification of novel HNRNPA1 mutation.

Hiroya Naruse¹, Hiroyuki Ishiura¹, Jun Mitsui¹, Hidetoshi Date¹, Yuji Takahashi², Takashi Matsukawa¹, Masaki Tanaka¹, Akiko Ishii³, Akira Tamaoka³, Keiichi Hokkoku⁴, Masahiro Sonoo⁴, Mari Segawa⁵, Yoshikazu Ugawa⁵, Koichiro Doi⁶, Jun Yoshimura⁶, Shinichi Morishita⁶, Jun Goto⁷, Shoji Tsuji⁸.

Abstract

To elucidate the genetic epidemiology of familial amyotrophic lateral sclerosis (FALS) in the Japanese population, we conducted whole-exome sequencing analysis of 30 FALS families in whom causative mutations have not been identified in previous studies. Consequently, whole-exome sequencing analysis revealed novel mutations in HNRNPA1, TBK1, and VCP. Taken together with our previous results of mutational analyses by direct nucleotide sequencing analysis, a microarray-based resequencing method, or repeat-primed PCR analysis, causative mutations were identified in 41 of the 68 families (60.3%) with SOD1 being the most frequent cause of FALS (39.7%). Of the mutations identified in this study, a novel c.862/1018C>G (p.P288A/340A) mutation in HNRNPA1 located in the nuclear localization signal domain of hnRNPA1, enhances the recruitment of mutant hnRNPA1 into stress granules, indicating that an altered nuclear localization signal activity plays an essential role in amyotrophic lateral sclerosis pathogenesis.

Entities: Disease Gene Mutation

Keywords: Familial amyotrophic lateral sclerosis; HNRNPA1; Stress granule; TBK1; VCP; Whole-exome sequencing analysis

Mesh：

Substances：

Year: 2017 PMID： 29033165 DOI： 10.1016/j.neurobiolaging.2017.08.030

Source DB: PubMed Journal: Neurobiol Aging ISSN： 0197-4580 Impact factor: 4.673

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Cited

12 in total

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Journal: Mol Genet Genomic Med Date: 2019-01-22 Impact factor: 2.183

Review 4. A Comprehensive Analysis of the Role of hnRNP A1 Function and Dysfunction in the Pathogenesis of Neurodegenerative Disease.

Authors: Joseph P Clarke; Patricia A Thibault; Hannah E Salapa; Michael C Levin
Journal: Front Mol Biosci Date: 2021-04-12

Review 5. Pathological phase transitions in ALS-FTD impair dynamic RNA-protein granules.

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6. Multiple Sclerosis-Associated hnRNPA1 Mutations Alter hnRNPA1 Dynamics and Influence Stress Granule Formation.

Authors: Joseph-Patrick W E Clarke; Patricia A Thibault; Hannah E Salapa; David E Kim; Catherine Hutchinson; Michael C Levin
Journal: Int J Mol Sci Date: 2021-03-12 Impact factor: 5.923

7. Dysregulation of RNA-Binding Proteins in Amyotrophic Lateral Sclerosis.

Authors: Yuan Chao Xue; Chen Seng Ng; Pinhao Xiang; Huitao Liu; Kevin Zhang; Yasir Mohamud; Honglin Luo
Journal: Front Mol Neurosci Date: 2020-05-29 Impact factor: 5.639

Review 8. ALS Genetics, Mechanisms, and Therapeutics: Where Are We Now?

Authors: Rita Mejzini; Loren L Flynn; Ianthe L Pitout; Sue Fletcher; Steve D Wilton; P Anthony Akkari
Journal: Front Neurosci Date: 2019-12-06 Impact factor: 4.677

Review 9. RNA-Binding Proteins and the Complex Pathophysiology of ALS.

Authors: Wanil Kim; Do-Yeon Kim; Kyung-Ha Lee
Journal: Int J Mol Sci Date: 2021-03-05 Impact factor: 5.923

10. Characterization of HNRNPA1 mutations defines diversity in pathogenic mechanisms and clinical presentation.

Authors: Danique Beijer; Hong Joo Kim; Lin Guo; Kevin O'Donovan; Inès Mademan; Tine Deconinck; Kristof Van Schil; Charlotte M Fare; Lauren E Drake; Alice F Ford; Andrzej Kochański; Dagmara Kabzińska; Nicolas Dubuisson; Peter Van den Bergh; Nicol C Voermans; Richard Jlf Lemmers; Silvère M van der Maarel; Devon Bonner; Jacinda B Sampson; Matthew T Wheeler; Anahit Mehrabyan; Steven Palmer; Peter De Jonghe; James Shorter; J Paul Taylor; Jonathan Baets
Journal: JCI Insight Date: 2021-07-22