Mutations in the gene PRRT2 cause paroxysmal kinesigenic dyskinesia with infantile convulsions.

Authors :: Lee HY
Huang Y
Bruneau N
Roll P
Roberson ED
Hermann M
Quinn E
Maas J
Edwards R
Ashizawa T
Baykan B
Bhatia K
Bressman S
Bruno MK
Brunt ER
Caraballo R
Echenne B
Fejerman N
Frucht S
Gurnett CA
Hirsch E
Houlden H
Jankovic J
Lee WL
Lynch DR
Mohammed S
Müller U
Nespeca MP
Renner D
Rochette J
Rudolf G
Saiki S
Soong BW
Swoboda KJ
Tucker S
Wood N
Hanna M
Bowcock AM
Szepetowski P
Fu YH
Ptáček LJ
Source :: Cell reports [Cell Rep] 2012 Jan 26; Vol. 1 (1), pp. 2-12. Date of Electronic Publication: 2011 Dec 15.
Publication Year :: 2012
Abstract: Paroxysmal kinesigenic dyskinesia with infantile convulsions (PKD/IC) is an episodic movement disorder with autosomal-dominant inheritance and high penetrance, but the causative genetic mutation is unknown. We have now identified four truncating mutations involving the gene PRRT2 in the vast majority (24/25) of well-characterized families with PKD/IC. PRRT2 truncating mutations were also detected in 28 of 78 additional families. PRRT2 encodes a proline-rich transmembrane protein of unknown function that has been reported to interact with the t-SNARE, SNAP25. PRRT2 localizes to axons but not to dendritic processes in primary neuronal culture, and mutants associated with PKD/IC lead to dramatically reduced PRRT2 levels, leading ultimately to neuronal hyperexcitability that manifests in vivo as PKD/IC.<br /> (Copyright © 2012 The Authors. Published by Elsevier Inc. All rights reserved.)

Full Text Access

Tools