Expanded Repeat in Canine Epilepsy

Author:

Lohi Hannes12345,Young Edwin J.12345,Fitzmaurice Susan N.12345,Rusbridge Clare12345,Chan Elayne M.12345,Vervoort Mike12345,Turnbull Julie12345,Zhao Xiao-Chu12345,Ianzano Leonarda12345,Paterson Andrew D.12345,Sutter Nathan B.12345,Ostrander Elaine A.12345,André Catherine12345,Shelton G. Diane12345,Ackerley Cameron A.12345,Scherer Stephen W.12345,Minassian Berge A.12345

Affiliation:

1. The Hospital for Sick Children, Toronto, Ontario M5G 1X8, Canada.

2. Wey Referrals, Woking, Surrey GU21 5BP, UK.

3. Stone Lion Veterinary Centre, Wimbledon, London SW19 5AU, UK.

4. Fred Hutchinson Cancer Research Center, Seattle, WA 98109–1024, USA.

5. CNRS Génétique et Développement, 35043 Rennes, France.

Abstract

Epilepsy afflicts 1% of humans and 5% of dogs. We report a canine epilepsy mutation and evidence for the existence of repeat-expansion disease outside humans. A canid-specific unstable dodecamer repeat in the Epm2b ( Nhlrc1 ) gene recurrently expands, causing a fatal epilepsy and contributing to the high incidence of canine epilepsy. Tracing the repeat origins revealed two successive events, starting 50 million years ago, unique to canid evolution. A genetic test, presented here, will allow carrier and presymptomatic diagnosis and disease eradication. Clinicopathologic characterization establishes affected animals as a model for Lafora disease, the most severe teenage-onset human epilepsy.

Publisher

American Association for the Advancement of Science (AAAS)

Subject

Multidisciplinary

Reference8 articles.

1. Materials and methods are available as supporting material on Science Online.

2. B. A. Minassian, Adv. Neurol.89, 199 (2002).

3. E. M. Chan et al., Neurology63, 565 (2004).

4. A. Weinhaeusel et al., Hum. Mutat.22, 404 (2003).

5. T. Saha, K. Usdin, FEBS Lett.491, 184 (2001).

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