Spinocerebellar Ataxia Type 8: Molecular Genetic Comparisons and Haplotype Analysis of 37 Families with Ataxia

Overview

Journal Am J Hum Genet

Publisher Cell Press

Specialty Genetics

Date 2004 May 21

PMID 15152344

Citations 27

Authors

Yoshio Ikeda

Joline C Dalton

Melinda L Moseley

Kathy L Gardner

Thomas D Bird

Tetsuo Ashizawa

William K Seltzer

Massimo Pandolfo

Aubrey Milunsky

Nicholas T Potter

Mikio Shoji

John B Vincent

John W Day

Laura P W Ranum

Affiliations

Soon will be listed here.

Abstract

We reported elsewhere that an untranslated CTG expansion causes the dominantly inherited neurodegenerative disorder spinocerebellar ataxia type 8 (SCA8). SCA8 shows a complex inheritance pattern with extremes of incomplete penetrance, in which often only one or two affected individuals are found in a given family. SCA8 expansions have also been found in control chromosomes, indicating that separate genetic or environmental factors increase disease penetrance among SCA8-expansion-carrying patients with ataxia. We describe the molecular genetic features and disease penetrance of 37 different families with SCA8 ataxia from the United States, Canada, Japan, and Mexico. Haplotype analysis using 17 STR markers spanning an approximately 1-Mb region was performed on the families with ataxia, on a group of expansion carriers in the general population, and on psychiatric patients, to clarify the genetic basis of the reduced penetrance and to investigate whether CTG expansions among different populations share a common ancestral background. Two major ancestrally related haplotypes (A and A') were found among white families with ataxia, normal controls, and patients with major psychosis, indicating a common ancestral origin of both pathogenic and nonpathogenic SCA8 expansions among whites. Two additional and distinct haplotypes were found among a group of Japanese families with ataxia (haplotype B) and a Mexican family with ataxia (haplotype C). Our finding that SCA8 expansions on three independently arising haplotypes are found among patients with ataxia and cosegregate with ataxia when multiple family members are affected further supports the direct role of the CTG expansion in disease pathogenesis.

Citing Articles

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The First Case of Spinocerebellar Ataxia Type 8 in Monozygotic Twins.

Sawada J, Katayama T, Tokashiki T, Kikuchi S, Kano K, Takahashi K Intern Med. 2019; 59(2):277-283.

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