0
Sep 2012, Vol 69, No. 9 >

Full Content is available to subscribers

Subscribe/Learn More
Original Contribution | Sep 2012

C9ORF72 Repeat Expansion in Amyotrophic Lateral Sclerosis in the Kii Peninsula of Japan

Hiroyuki Ishiura, MD, PhD; Yuji Takahashi, MD, PhD; Jun Mitsui, MD, PhD; Sohei Yoshida, MD, PhD; Tameko Kihira, MD, PhD; Yasumasa Kokubo, MD, PhD; Shigeki Kuzuhara, MD, PhD; Laura P. W. Ranum, PhD; Tomoko Tamaoki, MD, PhD; Yaeko Ichikawa, MD, PhD; Hidetoshi Date, PhD; Jun Goto, MD, PhD; Shoji Tsuji, MD, PhD
Arch Neurol. 2012;69(9):1154-1158. doi:10.1001/archneurol.2012.1219.
Text Size: A A A
Published online
Article
Figures
Tables
References
Comments

Background  In the Kii peninsula of Japan, high prevalences of amyotrophic lateral sclerosis (ALS) and parkinsonism-dementia complex have been reported. There are 2 major foci with a high prevalence, which include the southernmost region neighboring the Koza River (Kozagawa and Kushimoto towns in Wakayama prefecture) and the Hohara district (Mie prefecture).

Objective  To delineate the molecular basis of ALS in the Kii peninsula of Japan, we analyzed hexanucleotide repeat expansion in the chromosome 9 open reading frame 72 (C9ORF72) gene, which has recently been identified as a frequent cause of ALS and frontotemporal dementia in the white population.

Design  Case series.

Setting  University hospitals.

Patients  Twenty-one patients (1 familial patient and 20 sporadic patients) with ALS from Wakayama prefecture, and 16 patients with ALS and 16 patients with parkinsonism-dementia complex originating from Mie prefecture surveyed in 1994 through 2011 were enrolled in the study. In addition, 40 probands with familial ALS and 217 sporadic patients with ALS recruited from other areas of Japan were also enrolled in this study.

Main Outcome Measures  After screening by repeat-primed polymerase chain reaction, Southern blot hybridization analysis was performed to confirm the expanded alleles.

Results  We identified 3 patients with ALS (20%) with the repeat expansion in 1 of the 2 disease foci. The proportion is significantly higher than those in other regions in Japan. Detailed haplotype analyses revealed an extended shared haplotype in the 3 patients with ALS, suggesting a founder effect.

Conclusions  Our findings indicate that the repeat expansion partly accounts for the high prevalence of ALS in the Kii peninsula.
Figures in this Article

Sign In to Access Full Content

Don't have Access?

Register and get free email Table of Contents alerts, saved searches, PowerPoint downloads, CME quizzes, and more

Subscribe for full-text access to content from 1998 forward and a host of useful features

Activate your current subscription (AMA members and current subscribers)

Purchase Online Access to this article for 24 hours

Figures

Place holder to copy figure label and caption
Grahic Jump Location
+Image not available.
View Large  |  Save Figure  |  Download Slide (.ppt)  |  View in Article Context
Image not available.

Figure 1. Map of Kii peninsula of Japan and distribution of patients with amyotrophic lateral sclerosis (ALS) and parkinsonism-dementia complex (PDC). The southernmost area neighboring the Koza River (Kozagawa and Kushimoto towns) and the Hohara district and its vicinity (Minamiise town and Shima city) shown in the figure are 2 disease foci. The circles represent examined patients with ALS. The filled-in circles designate patients with the repeat expansion in C9ORF72. The triangles represent patients with the PDC phenotype. Each symbol indicates the proband in the family when multiple affected family members were observed. Patients with hexanucleotide repeat expansion in C9ORF72 are concentrated in the southernmost Kii peninsula.

Place holder to copy figure label and caption
Grahic Jump Location
+Image not available.
View Large  |  Save Figure  |  Download Slide (.ppt)  |  View in Article Context
Image not available.

Figure 2. Mutational analyses of hexanucleotide repeat expansion in C9ORF72. A, Repeat-primed polymerase chain reaction analysis was performed as previously described.8 Patients 1-3 show the characteristic sawtooth patterns with a 6-bp periodicity (blue lines). Red lines indicate DNA size markers. B, Southern blot hybridization analysis. Genomic DNA extracted from lymphoblastoid cell lines of patients 1 through 3 were subjected to Southern blot hybridization analysis, as described previously.12 Patients 1-3 showed expanded alleles. C, Result of haplotype analysis. Physical positions are shown using the reference genome (NCBI36/hg18). An extended haplotype (Kii 9p-haplotype) spanning 3.3-63 Mb was shared by the 3 patients with ALS with the repeat expansions. A 410-kb region (defined by rs911602 and rs10511810) of the Kii 9p-haplotype was shared with that in another patient with the repeat expansion from another region of Japan.14 We compared this haplotype with the Finnish haplotype; a 130-kb region (defined by rs10511816 and rs633583) was shared between the Kii 9p-haplotype and the Finnish haplotype. NC indicates negative control; P, patient.

Tables

Interactive Graphics

Video

Country-Specific Mortality and Growth Failure in Infancy and Yound Children and Association With Material Stature

Use interactive graphics and maps to view and sort country-specific infant and early dhildhood mortality and growth failure data and their association with maternal

References

Correspondence

Submit a Letter
CME
Accreditation Information
The American Medical Association is accredited by the Accreditation Council for Continuing Medical Education to provide continuing medical education for physicians. The AMA designates this journal-based CME activity for a maximum of 1 AMA PRA Category 1 CreditTM per course. Physicians should claim only the credit commensurate with the extent of their participation in the activity. Physicians who complete the CME course and score at least 80% correct on the quiz are eligible for AMA PRA Category 1 CreditTM.
Note: You must get at least of the answers correct to pass this quiz.
Clear Answers | Save For Later
You have not filled in all the answers to complete this quiz
The following questions were not answered:
Sorry, you have unsuccessfully completed this CME quiz with a score of
The following questions were not answered correctly:
Commitment to Change (optional):
Indicate what change(s) you will implement in your practice, if any, based on this CME course.
Your quiz results:
The filled radio buttons indicate your responses. The preferred responses are highlighted
For CME Course: A Proposed Model for Initial Assessment and Management of Acute Heart Failure Syndromes
Indicate what changes(s) you will implement in your practice, if any, based on this CME course.
NOTE:
Citing articles are presented as examples only. In non-demo SCM6 implementation, integration with CrossRef’s “Cited By” API will populate this tab (http://www.crossref.org/citedby.html).
Compression-Only CPR: Pushing the Science Forward
Cone
AAM 2010;304:1493-1495.
All you need to read in the other general journals
BMJ 2010;341:c5893-c1494.
Submit a Comment

Some tools below are only available to our subscribers or users with an online account.

Web of Science® Times Cited: 1

Sign In to Access Full Content

Related Content

Customize your page view by dragging & repositioning the boxes below.

Articles Related By Topic
Related Topics
PubMed Articles
Protein aggregation in amyotrophic lateral sclerosis.
Acta Neuropathol Published online May 15, 2013.;
Mutation analysis and immunopathological studies of PFN1 in familial and sporadic amyotrophic lateral sclerosis.
Neurobiol Aging Published online Apr 28, 2013.;
Jobs

More Listings at
JAMACareerCenter.com >

© 2013 American Medical Association. All Rights Reserved.
Powered bySilverchair Information Systems