A novel mutation in KCNA1 causes episodic ataxia without myokymia.

Hane Lee; Hui Wang; Joanna C. Jen; Chiara Sabatti; Robert W. Baloh; Stanley F. Nelson

doi:10.1002/humu.9295

A novel mutation in KCNA1 causes episodic ataxia without myokymia.

Hane Lee
, Hui Wang
, Joanna C. Jen
, Chiara Sabatti
, Robert W. Baloh
, Stanley F. Nelson

Research output: Contribution to journal › Article › peer-review

47 Scopus citations

Abstract

We describe a unique family in which several individual are affected with episodes of ataxia that best fit the phenotype of episodic ataxia type 2 (EA2). All of the affected family members had episodes typically lasting for several hours, and none of them had muscle abnormalities including myokymia. Episodic ataxia type 1 (EA1) was not considered initially as a clinical diagnosis for the affected individuals in this family. However, by linkage mapping, sequencing and polymorphism analysis, all affecteds were found to have a novel mutation in KCNA1. Numerous missense mutations have been described previously in KCNA1 that cause EA1. The mutation c.1025G>T replaces a highly conserved serine with isoleucine at position 342 (p.Ser342Ile) in the highly conserved fifth transmembrane domain of the KCNA1. This mutation leads to a distinct clinical phenotype without myokymia broadening the scope of clinical characteristics of EA1 and highlighting the heterogeneity of phenotypic effects from distinct missense mutations.

Original language	English
Pages (from-to)	536
Number of pages	1
Journal	Human Mutation
Volume	24
Issue number	6
DOIs	https://doi.org/10.1002/humu.9295
State	Published - Dec 2004
Externally published	Yes

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title = "A novel mutation in KCNA1 causes episodic ataxia without myokymia.",

abstract = "We describe a unique family in which several individual are affected with episodes of ataxia that best fit the phenotype of episodic ataxia type 2 (EA2). All of the affected family members had episodes typically lasting for several hours, and none of them had muscle abnormalities including myokymia. Episodic ataxia type 1 (EA1) was not considered initially as a clinical diagnosis for the affected individuals in this family. However, by linkage mapping, sequencing and polymorphism analysis, all affecteds were found to have a novel mutation in KCNA1. Numerous missense mutations have been described previously in KCNA1 that cause EA1. The mutation c.1025G>T replaces a highly conserved serine with isoleucine at position 342 (p.Ser342Ile) in the highly conserved fifth transmembrane domain of the KCNA1. This mutation leads to a distinct clinical phenotype without myokymia broadening the scope of clinical characteristics of EA1 and highlighting the heterogeneity of phenotypic effects from distinct missense mutations.",

author = "Hane Lee and Hui Wang and Jen, \{Joanna C.\} and Chiara Sabatti and Baloh, \{Robert W.\} and Nelson, \{Stanley F.\}",

year = "2004",

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T1 - A novel mutation in KCNA1 causes episodic ataxia without myokymia.

AU - Lee, Hane

AU - Wang, Hui

AU - Jen, Joanna C.

AU - Sabatti, Chiara

AU - Baloh, Robert W.

AU - Nelson, Stanley F.

PY - 2004/12

Y1 - 2004/12

N2 - We describe a unique family in which several individual are affected with episodes of ataxia that best fit the phenotype of episodic ataxia type 2 (EA2). All of the affected family members had episodes typically lasting for several hours, and none of them had muscle abnormalities including myokymia. Episodic ataxia type 1 (EA1) was not considered initially as a clinical diagnosis for the affected individuals in this family. However, by linkage mapping, sequencing and polymorphism analysis, all affecteds were found to have a novel mutation in KCNA1. Numerous missense mutations have been described previously in KCNA1 that cause EA1. The mutation c.1025G>T replaces a highly conserved serine with isoleucine at position 342 (p.Ser342Ile) in the highly conserved fifth transmembrane domain of the KCNA1. This mutation leads to a distinct clinical phenotype without myokymia broadening the scope of clinical characteristics of EA1 and highlighting the heterogeneity of phenotypic effects from distinct missense mutations.

AB - We describe a unique family in which several individual are affected with episodes of ataxia that best fit the phenotype of episodic ataxia type 2 (EA2). All of the affected family members had episodes typically lasting for several hours, and none of them had muscle abnormalities including myokymia. Episodic ataxia type 1 (EA1) was not considered initially as a clinical diagnosis for the affected individuals in this family. However, by linkage mapping, sequencing and polymorphism analysis, all affecteds were found to have a novel mutation in KCNA1. Numerous missense mutations have been described previously in KCNA1 that cause EA1. The mutation c.1025G>T replaces a highly conserved serine with isoleucine at position 342 (p.Ser342Ile) in the highly conserved fifth transmembrane domain of the KCNA1. This mutation leads to a distinct clinical phenotype without myokymia broadening the scope of clinical characteristics of EA1 and highlighting the heterogeneity of phenotypic effects from distinct missense mutations.

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DO - 10.1002/humu.9295

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JO - Human Mutation

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ER -

A novel mutation in KCNA1 causes episodic ataxia without myokymia.

Abstract

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