Paralogue Annotation for CACNA1C residue 701

Residue details

Gene: CACNA1C
Reference Sequences: LRG: LRG_334, Ensembl variant: ENST00000399655 / ENSP00000382563
Amino Acid Position: 701
Reference Amino Acid: Q - Glutamine
Protein Domain: TM domain 2


Paralogue Variants mapped to CACNA1C residue 701

ParalogueVariantAssociated DiseaseMapping QualityConsensusPubmed
SCN5AR893CBrugada syndromeMedium9 20129283, 24136861
SCN5AR893HBrugada syndromeMedium9 20129283, 24136861
SCN1AR946SGeneralized epilepsy of infancyMedium9 15944908
SCN1AR946CMyoclonic epilepsy of infancyMedium9 14738421, 21864321, 23195492, 24168886
SCN1AR946HMyoclonic epilepsy of infancyMedium9 14738421, 21371021, 21864321, 23195492
SCN2AR937CIntellectual disability, nonsyndromicMedium9 23020937
SCN1AR946PDravet syndromeMedium9 24168886
SCN10AR844HBrugada syndromeMedium9 25842276

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 CACNA1C.



CACNA1C-----------MQTRRSTFDNFPQSLLTVF>Q<ILTGEDWNSVMYDGIMAYGGPSFPGMLVCI731
CACNA1A-----------G-TPPTNFDTFPAAIMTVF>Q<ILTGEDWNEVMYDGIKSQGGV-QGGMVFSI692
CACNA1B-----------E-TPTTNFDTFPAAILTVF>Q<ILTGEDWNAVMYHGIESQGGV-SKGMFSSF688
CACNA1D-----------TQTKRSTFDNFPQALLTVF>Q<ILTGEDWNAVMYDGIMAYGGPSSSGMIVCI750
CACNA1E-----------G-TPSANFDTFPAAIMTVF>Q<ILTGEDWNEVMYNGIRSQGGV-SSGMWSAI681
CACNA1F-----------THTKRSTFDTFPQALLTVF>Q<ILTGEDWNVVMYDGIMAYGGPFFPGMLVCI736
CACNA1G-------DG-DTLPDRKNFDSLLWAIVTVF>Q<ILTQEDWNKVLYNGMAS-T-S----SWAAL942
CACNA1H-------TG-DTVPDRKNFDSLLWAIVTVF>Q<ILTQEDWNVVLYNGMAS-T-S----SWAAL993
CACNA1I-------TG-DTVPDRKNFDSLLWAIVTVF>Q<ILTQEDWNVVLYNGMAS-T-S----PWASL840
CACNA1S-----------TEVRRSNFDNFPQALISVF>Q<VLTGEDWTSMMYNGIMAYGGPSYPGMLVCI639
SCN10AN----I-SAPHEDWPRWHMHDFFHSFLIVF>R<ILCGE-WIENMWACMEV-----GQKSICLI868
SCN11APKLCNPTGPTVSCLRHWHMGDFWHSFLVVF>R<ILCGE-WIENMWECMQEAN---ASSSLCVI789
SCN1AK----I-AS-DCQLPRWHMNDFFHSFLIVF>R<VLCGE-WIETMWDCMEV-----AGQAMCLT970
SCN2AK----I-SN-DCELPRWHMHDFFHSFLIVF>R<VLCGE-WIETMWDCMEV-----AGQTMCLT961
SCN3AK----I-ND-DCTLPRWHMNDFFHSFLIVF>R<VLCGE-WIETMWDCMEV-----AGQTMCLI962
SCN4AK----I-AL-DCNLPRWHMHDFFHSFLIVF>R<ILCGE-WIETMWDCMEV-----AGQAMCLT780
SCN5AS----D-SG---LLPRWHMMDFFHAFLIIF>R<ILCGE-WIETMWDCMEV-----SGQSLCLL917
SCN7AH----I-DK-DCQLPRWHMHDFFHSFLNVF>R<ILCGE-WVETLWDCMEV-----AGQSWCIP707
SCN8AK----I-NQ-DCELPRWHMHDFFHSFLIVF>R<VLCGE-WIETMWDCMEV-----AGQAMCLI955
SCN9AK----I-ND-DCTLPRWHMNDFFHSFLIVF>R<VLCGE-WIETMWDCMEV-----AGQAMCLI935
cons                              > <                              

See full Alignment of Paralogues


Known Variants in CACNA1C

There are currently no reported variants at residue 701 for CACNA1C.