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Identification and characterization of a novel genetic mutation with prolonged QT syndrome in an unexplained postoperative death.

Authors :
Hata, Yukiko
Mori, Hisashi
Tanaka, Ayumi
Fujita, Yosuke
Shimomura, Takeshi
Tabata, Toshihide
Kinoshita, Koshi
Yamaguchi, Yoshiaki
Ichida, Fukiko
Kominato, Yoshihiko
Ikeda, Noriaki
Nishida, Naoki
Source :
International Journal of Legal Medicine. Jan2014, Vol. 128 Issue 1, p105-115. 11p.
Publication Year :
2014

Abstract

Introduction: The human ether- à- go- go-related gene ( hERG) encodes the α-subunit of a cardiac potassium channel. Various mutations of hERG, including missense mutations, have been reported to cause long QT syndrome (LQTS) and severe arrhythmic disorders such as sudden cardiac death. We identified a novel hERG frameshift mutation ( hERG(ΔAT)) in the S5-pore region from a LQTS patient who died suddenly and analyzed its genetic profile and the molecular and electrophysiological behaviors of the protein product to assess the pathogenicity of hERG(ΔAT). Methods and results: We performed direct sequencing of hERG and evaluated its transcript level by using a whole blood sample from the patient. We performed immunoblotting, immunocytochemistry, and patch-clamp recordings of HEK-293 T cells transfected with hERG(ΔAT), wild-type hERG ( hERG(WT)), or both. The patient demonstrated an AT deletion (c.1735_1736del) in hERG and a decrease in hERG mRNA transcripts. HEK-293 T cells showed lower production and cell surface expression of hERG(ΔAT) compared with hERG(WT) protein. In addition, the hERG(∆AT) protein failed to form functional channels, while the activation kinetics of functional channels, presumably consisting of hERG(WT) subunits, were unaffected. Conclusion: The ΔAT mutation may decrease the number of functional hERG channels by impairing the posttranscriptional and posttranslational processing of the mutant product. This decrease may partly explain the cardiac symptoms of the patient who was heterozygous for hERG(ΔAT). [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
09379827
Volume :
128
Issue :
1
Database :
Academic Search Index
Journal :
International Journal of Legal Medicine
Publication Type :
Academic Journal
Accession number :
93392461
Full Text :
https://doi.org/10.1007/s00414-013-0853-4