Autosomal recessive long-QT syndrome (Jervell Lange-Nielsen syndrome) is genetically heterogeneous |
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| Authors: | E. Schulze-Bahr W. Haverkamp H. Wedekind C. Rubie M. Hördt M. Borggrefe G. Assmann G. Breithardt H. Funke |
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| Affiliation: | (1) Department of Cardiology and Angiology, Hospital of the University of Münster, D-48129 Münster, Germany, DE;(2) Institute for Arteriosclerosis Research at the University of Münster, Domagkstrasse 3, D-48145 Münster, Germany, DE |
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| Abstract: | Jervell Lange-Nielsen syndrome (JLNS) is a recessive disorder with congenital deafness and long-QT syndrome (LQTS). Mutations in the potassium-channel gene KVLQT1 (LQTS 1) have been identified in JLNS and in autosomal-dominant LQTS as well. We performed haplotype analysis with microsatellite markers in a Lebanese family with JLNS, but failed to detect linkage at LQTS 1. Moreover, using this approach, we excluded two other ion-channel genes involved in autosomal-dominant LQTS, HERG (LQTS 2) and SCN5A (LQTS 3). Our findings indicate that JLNS is genetically heterogeneous and that, in this family, an unknown LQTS gene causes the disease. Received: 19 September 1995 / Accepted: 15 May 1997 |
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