Presence of Alanine-to-valine Substitutions in Myofibrillogenesis Regulator 1 in Paroxysmal Nonkinesigenic Dyskinesia: Confirmation in 2 Kindreds

Overview

Journal Arch Neurol

Specialty Neurology

Date 2005 Apr 13

PMID 15824259

Citations 15

Authors

Dong-Hui Chen

Mark Matsushita

Shirley Rainier

Brandon Meaney

Lisa Tisch

Abreham Feleke

John Wolff

Hillary Lipe

John Fink

Thomas D Bird

Wendy H Raskind

Affiliations

Soon will be listed here.

Abstract

Background: Paroxysmal nonkinesigenic dyskinesia (PNKD) is a rare disorder characterized by attacks of involuntary movements brought on by stress, alcohol, or caffeine, but not by movement. An autosomal dominant form of this disorder was mapped to chromosome 2q33-36, and different missense mutations in exon 1 of the myofibrillogenesis regulator 1 (MR1) gene were identified recently in 2 kindreds.

Objectives: To describe studies on a new pedigree with PNKD, to explore the possibility of locus heterogeneity, and to further delineate the spectrum of mutations in MR1 in 2 families with PNKD.

Design, Setting, And Patients: All 10 exons of MR1 were sequenced in DNA from members of 2 pedigrees with autosomal dominant PNKD.

Results: Different missense mutations in exon 1 of MR1 that cosegregate with disease were identified in each multiplex family. These single-nucleotide mutations predicted substitution of valine for alanine in residue 7 in one family and residue 9 in the other. The same mutations were found in the only 2 families previously published. Family history and haplotype analysis make it unlikely that the families with the same mutations are related.

Conclusions: The function of MR1 is unknown, but the 2 mutations identified in the 4 families with PNKD studied to date are predicted to disrupt the amino terminal alpha-helix suggesting that this region of the gene is critical for proper gene function under stressful conditions. Study of additional families will be important to determine whether analysis of a single exon (MR1 exon 1) is sufficient for genetic testing purposes.

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