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Refined localisation of the voltage-gated chloride channel, CLCN3, to 4q33.

作者信息

Taine L, Coupry I, Boisseau P, Saura R, Lacombe D, Arveiler B

机构信息

Laboratoire de Pathologie Moléculaire et Thérapie Génique, Université Victor Segalen Bordeaux, France.

出版信息

Hum Genet. 1998 Feb;102(2):178-81. doi: 10.1007/s004390050673.

Abstract

Mutations in ion channels have been shown to be responsible for a variety of neurological and muscular diseases. The voltage-gated chloride channel CLCN3 was recently mapped to chromosomal region 4q32. We are analysing a young female patient with Wolf-Hirschhorn syndrome and chorea associated with an inversion-deletion of chromosome 4 [46XX,inv(4)del(4)(qter-->q33::p15.32-->q33]. Considering that chorea in this patient might be due to the disruption of a gene at either of the 4p15.32 or 4q33 breakpoints, CLCN3 was considered as a candidate gene. We showed by FISH analysis with a CLCN3 YAC that the gene was not broken by the inv-del event, and was therefore an unlikely candidate. Using high resolution techniques, we refined the localisation of CLCN3 to 4q33.

摘要

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