Paralogue Annotation for KCNH2 residue 657

Residue details

Gene: KCNH2
Reference Sequences: LRG: LRG_288, Ensembl variant: ENST00000262186 / ENSP00000262186
Amino Acid Position: 657
Reference Amino Acid: G - Glycine
Protein Domain: Transmembrane/Linker/Pore


Paralogue Variants mapped to KCNH2 residue 657

ParalogueVariantAssociated DiseaseMapping QualityConsensusPubmed
CNGA3G397VAchromatopsiaHigh9 18636117
KCNH1G496RZimmermann-Laband syndromeHigh9 25915598, 25915598
KCNH1G496EHypotonia, seizures and developmental delayHigh9 26818738

To assess whether the paralogue annotation here confidently predicts that variation at this residue is pathogenic, it is important to check the reports in the Pubmed links above to ascertain that the mutations in these paralogues have been proved likely to be disease-causing. It is also important to check that the direction of effect of the variant in the paralogue is compatible with your observed phenotype in KCNH2.



KCNH2FGNVSPNTNSEKIFSICVMLIGSLMYASIF>G<NVSAIIQRLYSGTARYHTQMLRVREFIRFH687
KCNH1FGNIAPSTDIEKIFAVAIMMIGSLLYATIF>G<NVTTIFQQMYANTNRYHEMLNSVRDFLKLY526
KCNH3FGNVSANTDTEKIFSICTMLIGALMHAVVF>G<NVTAIIQRMYARRFLYHSRTRDLRDYIRIH528
KCNH4FGNVCANTDAEKIFSICTMLIGALMHAVVF>G<NVTAIIQRMYSRRSLYHSRMKDLKDFIRVH502
KCNH5FGNIAPTTDVEKMFSVAMMMVGSLLYATIF>G<NVTTIFQQMYANTNRYHEMLNNVRDFLKLY495
KCNH6FGNVSPNTNSEKVFSICVMLIGSLMYASIF>G<NVSAIIQRLYSGTARYHTQMLRVKEFIRFH539
KCNH7FGNVSPNTNSEKIFSICVMLIGSLMYASIF>G<NVSAIIQRLYSGTARYHMQMLRVKEFIRFH690
KCNH8FGNVSANTDAEKIFSICTMLIGALMHALVF>G<NVTAIIQRMYSRWSLYHTRTKDLKDFIRVH497
CNGA1-ETPPPVRDSEYVFVVVDFLIGVLIFATIV>G<NIGSMISNMNAARAEFQARIDAIKQYMHFR424
CNGA2-ETPPPVKDEEYLFVIFDFLIGVLIFATIV>G<NVGSMISNMNATRAEFQAKIDAVKHYMQFR399
CNGA3-ETPPPVKDEEYLFVVVDFLVGVLIFATIV>G<NVGSMISNMNASRAEFQAKIDSIKQYMQFR427
CNGA4-DTPPPAREEEYLFMVGDFLLAVMGFATIM>G<SMSSVIYNMNTADAAFYPDHALVKKYMKLQ293
CNGB1-GLPDPKTLFEIVFQLLNYFTGVFAFSVMI>G<QMRDVVGAATAGQTYYRSCMDSTVKYMNFY907
CNGB3-GLPEPQTLFEIVFQLLNFFSGVFVFSSLI>G<QMRDVIGAATANQNYFRACMDDTIAYMNNY469
HCN1YGAQAPVSMSDLWITMLSMIVGATCYAMFV>G<HATALIQSLDSSRRQYQEKYKQVEQYMSFH421
HCN2YGRQAPESMTDIWLTMLSMIVGATCYAMFI>G<HATALIQSLDSSRRQYQEKYKQVEQYMSFH490
HCN3YGQQAPVGMPDVWLTMLSMIVGATCYAMFI>G<HATALIQSLDSSRRQYQEKYKQVEQYMSFH374
HCN4YGRQAPVGMSDVWLTMLSMIVGATCYAMFI>G<HATALIQSLDSSRRQYQEKYKQVEQYMSFH541
cons                              > <                              

See full Alignment of Paralogues


Known Variants in KCNH2

ProteinCDSDisease ClassificationDiseasedbSNP linksEffect Prediction
p.G657Cc.1969G>T Inherited ArrhythmiaLQTSrs199472978SIFT: deleterious
Polyphen: probably damaging
ReportsInherited ArrhythmiaLQTS [DNA-based diagnostics of long QT syndrome]. Tidsskr Nor Laegeforen. 2005 125(20):2783-6. 16244680
Inherited ArrhythmiaLQTS Molecular genetic analysis of long QT syndrome in Norway indicating a high prevalence of heterozygous mutation carriers. Scand J Clin Lab Invest. 2008 68(5):362-8. 18752142
Inherited ArrhythmiaLQTS The genetic basis of long QT and short QT syndromes: a mutation update. Hum Mutat. 2009 30(11):1486-511. 19862833
p.G657Rc.1969G>C Inherited ArrhythmiaLQTSrs199472978SIFT: deleterious
Polyphen: probably damaging
ReportsInherited ArrhythmiaLQTS Spectrum and prevalence of mutations from the first 2,500 consecutive unrelated patients referred for the FAMILION long QT syndrome genetic test. Heart Rhythm. 2009 6(9):1297-303. 19716085
Inherited ArrhythmiaLQTS Large-scale mutational analysis of Kv11.1 reveals molecular insights into type 2 long QT syndrome. Nat Commun. 2014 5:5535. doi: 10.1038/ncomms6535. 25417810
p.G657Sc.1969G>A Inherited ArrhythmiaLQTSrs199472978SIFT: deleterious
Polyphen: probably damaging
ReportsInherited ArrhythmiaLQTS Spectrum and prevalence of mutations from the first 2,500 consecutive unrelated patients referred for the FAMILION long QT syndrome genetic test. Heart Rhythm. 2009 6(9):1297-303. 19716085