Whole-exome sequencing identifies a missense mutation in hnRNPA1 in a family with flail arm ALS

Qing Liu; Shi Shu; Rong Rong Wang; Fang Liu; Bo Cui; Xia Nan Guo; Chao Xia Lu; Xiao Guang Li; Ming Sheng Liu; Bin Peng; Li-Ying Cui; Xue Zhang

doi:10.1212/WNL.0000000000003256

Whole-exome sequencing identifies a missense mutation in hnRNPA1 in a family with flail arm ALS

Neurology. 2016 Oct 25;87(17):1763-1769. doi: 10.1212/WNL.0000000000003256. Epub 2016 Sep 30.

Authors

Qing Liu¹, Shi Shu¹, Rong Rong Wang¹, Fang Liu¹, Bo Cui¹, Xia Nan Guo¹, Chao Xia Lu¹, Xiao Guang Li¹, Ming Sheng Liu¹, Bin Peng¹, Li-Ying Cui¹, Xue Zhang²

Affiliations

¹ From the Department of Neurology and Laboratory of Clinical Genetics, Peking Union Medical College Hospital (Q.L., B.C., X.G.L., M.S.L., B.P., L.-y.C., X.Z.), and McKusick-Zhang Center for Genetic Medicine (S.S., R.R.W., F.L., X.N.G., C.X.L., X.Z.), Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing; and Neuroscience Center (Q.L., S.S., R.R.W., F.L., B.C., X.N.G., C.X.L., X.G.L., M.S.L., B.P., L.-y.C., X.Z.), Chinese Academy of Medical Sciences, Beijing, China.
² From the Department of Neurology and Laboratory of Clinical Genetics, Peking Union Medical College Hospital (Q.L., B.C., X.G.L., M.S.L., B.P., L.-y.C., X.Z.), and McKusick-Zhang Center for Genetic Medicine (S.S., R.R.W., F.L., X.N.G., C.X.L., X.Z.), Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing; and Neuroscience Center (Q.L., S.S., R.R.W., F.L., B.C., X.N.G., C.X.L., X.G.L., M.S.L., B.P., L.-y.C., X.Z.), Chinese Academy of Medical Sciences, Beijing, China. xuezhang@pumc.edu.cn.

PMID: 27694260
DOI: 10.1212/WNL.0000000000003256

Abstract

Objective: To identify the disease-causing gene of a family with upper limb predominant, slowly progressive amyotrophic lateral sclerosis (ALS), which was diagnosed as flail arm syndrome (FAS).

Methods: After causation of 24 known ALS genes was excluded by targeted next-generation sequencing, whole-exome sequencing was applied in the FAS family. Cellular localization of mutant hnRNPA1 was examined in transfected HeLa cells. An additional 251 Chinese patients with ALS (including 7 sporadic FAS) underwent mutation screening of hnRNPA1.

Results: We detected a novel missense mutation in hnRNPA1, c.862/1018C>T (p.P288S/P340S), which cosegregated with disease in the FAS family. The residue is highly conserved across species and exists in the encoded PY nuclear localization signal of hnRNPA1 protein. Mutant hnRNPA1 showed altered intracellular localization, resulting in formation of cytoplasmic inclusions that colocalized with stress granules in transfected cells. Further mutation screening of hnRNPA1 in additional patients with FAS and typical ALS detected 2 rare variants with unknown significance. These variants lie in the prion-like domain of hnRNPA1 long isoform, which was detected exclusively in the CNS.

Conclusions: Our results suggest that hnRNPA1 is the causative gene in the family with flail arm ALS. This further expanded the disease phenotype of hnRNPA1 mutations.

MeSH terms

Adult
Aged
Amyotrophic Lateral Sclerosis / genetics*
Amyotrophic Lateral Sclerosis / pathology*
Arm / physiopathology*
Exome / genetics
Family Health
Female
Genetic Predisposition to Disease / genetics*
Heterogeneous Nuclear Ribonucleoprotein A1
Heterogeneous-Nuclear Ribonucleoprotein Group A-B / genetics*
Humans
Kv1.5 Potassium Channel / genetics
Male
Mutation, Missense / genetics*
Severity of Illness Index

Substances

Heterogeneous Nuclear Ribonucleoprotein A1
Heterogeneous-Nuclear Ribonucleoprotein Group A-B
Kv1.5 Potassium Channel
hnRNPA1 protein, human