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Long QT syndrome and life threatening arrhythmia in a newborn: molecular diagnosis and treatment response.


ABSTRACT: Intrauterine and neonatal manifestations of congenital long QT syndrome are associated with a high cardiac risk, particularly when atrioventricular block and excessive QT prolongation (> 600 ms(1/2)) are present. In a female newborn with these features, treatment with propranolol and mexiletine led to complete reduction of arrhythmia that was maintained 1.5 years later. High throughput genetic analysis found a sodium channel gene (LQT3) mutation. Disappearance of the 2:1 atrioventricular block and QTc shortening (from 740 ms(1/2) to 480 ms(1/2)), however, was achieved when mexiletine was added to propranolol. This effect was considered to be possibly genotype related. Early onset forms of long QT syndrome may benefit from advanced genotyping.

SUBMITTER: Schulze-Bahr E 

PROVIDER: S-EPMC1768001 | biostudies-literature | 2004 Jan

REPOSITORIES: biostudies-literature

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Long QT syndrome and life threatening arrhythmia in a newborn: molecular diagnosis and treatment response.

Schulze-Bahr E E   Fenge H H   Etzrodt D D   Haverkamp W W   Mönnig G G   Wedekind H H   Breithardt G G   Kehl H-G HG  

Heart (British Cardiac Society) 20040101 1


Intrauterine and neonatal manifestations of congenital long QT syndrome are associated with a high cardiac risk, particularly when atrioventricular block and excessive QT prolongation (> 600 ms(1/2)) are present. In a female newborn with these features, treatment with propranolol and mexiletine led to complete reduction of arrhythmia that was maintained 1.5 years later. High throughput genetic analysis found a sodium channel gene (LQT3) mutation. Disappearance of the 2:1 atrioventricular block a  ...[more]

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