Drug-induced long QT syndrome (LQTs) is a prevalent disorder of uncertain e
tiology that predisposes to sudden death. KCNE2 encodes MinK-related peptid
e 1 (MiRP1), a subunit of the cardiac potassium channel I-Kr that has been
associated previously with inherited LQTS, Here, we examine KCNE2 in 98 pat
ients with drug-induced LQTs, identifying three individuals with sporadic m
utations and a patient with sulfamethoxazole-associated LQTs who carried a
single-nucleotide polymorphism (SNP) found in approximate to 1.6% of the ge
neral population. While mutant channels showed diminished potassium flux at
baseline and wild-type drug sensitivity, channels with the SNP were normal
at baseline but inhibited by sulfamethoxazole at therapeutic levels that d
id not affect wild-type channels. We conclude that allelic variants of MiRP
1 contribute to a significant fraction of cases of drug-induced LQTs throug
h multiple mechanisms and that common sequence variations that increase the
risk of life-threatening drug reactions can be clinically silent before dr
ug exposure.