BACKGROUND: Brugada syndrome (BrS) is associated with mutations in the cardiac sodium channel (Na(v)1.5). We previously reported that the function of a trafficking-deficient BrS Na(v)1.5 mutation, R282H, could be restored by coexpression with the sodium channel polymorphism H558R. Here, we tested the hypothesis that peptide fragments from Na(v)1.5, spanning the H558R polymorphism, can be used to restore trafficking of trafficking-deficient BrS sodium channel mutations. METHODS AND RESULTS: Whole-cell patch clamping revealed that cotransfection in human embryonic kidney (HEK293) cells of the R282H channel with either the 40- or 20-amino acid cDNA fragments of Na(v)1.5 containing the H558R polymorphism restored trafficking of this mutant channel. Fluorescence resonance energy transfer suggested that the trafficking-deficient R282H channel was misfolded, and this was corrected on coexpression with R558-containing peptides that restored trafficking of the R282H channel. Importantly, we also expressed the peptide spanning the H558R polymorphism with 8 additional BrS Na(v)1.5 mutations with reduced currents and demonstrated that the peptide was able to restore significant sodium currents in 4 of them. CONCLUSIONS: In the present study, we demonstrate that small peptides, spanning the H558R polymorphism, are sufficient to restore the trafficking defect of BrS-associated Na(v)1.5 mutations. Our findings suggest that it might be possible to use short cDNA constructs as a novel strategy tailored to specific disease-causing mutants of BrS.
BACKGROUND:Brugada syndrome (BrS) is associated with mutations in the cardiac sodium channel (Na(v)1.5). We previously reported that the function of a trafficking-deficient BrS Na(v)1.5 mutation, R282H, could be restored by coexpression with the sodium channel polymorphism H558R. Here, we tested the hypothesis that peptide fragments from Na(v)1.5, spanning the H558R polymorphism, can be used to restore trafficking of trafficking-deficient BrS sodium channel mutations. METHODS AND RESULTS: Whole-cell patch clamping revealed that cotransfection in humanembryonic kidney (HEK293) cells of the R282H channel with either the 40- or 20-amino acid cDNA fragments of Na(v)1.5 containing the H558R polymorphism restored trafficking of this mutant channel. Fluorescence resonance energy transfer suggested that the trafficking-deficient R282H channel was misfolded, and this was corrected on coexpression with R558-containing peptides that restored trafficking of the R282H channel. Importantly, we also expressed the peptide spanning the H558R polymorphism with 8 additional BrS Na(v)1.5 mutations with reduced currents and demonstrated that the peptide was able to restore significant sodium currents in 4 of them. CONCLUSIONS: In the present study, we demonstrate that small peptides, spanning the H558R polymorphism, are sufficient to restore the trafficking defect of BrS-associated Na(v)1.5 mutations. Our findings suggest that it might be possible to use short cDNA constructs as a novel strategy tailored to specific disease-causing mutants of BrS.
Authors: C Bezzina; M W Veldkamp; M P van Den Berg; A V Postma; M B Rook; J W Viersma; I M van Langen; G Tan-Sindhunata; M T Bink-Boelkens; A H van Der Hout; M M Mannens; A A Wilde Journal: Circ Res Date: 1999 Dec 3-17 Impact factor: 17.367
Authors: R Dumaine; J A Towbin; P Brugada; M Vatta; D V Nesterenko; V V Nesterenko; J Brugada; R Brugada; C Antzelevitch Journal: Circ Res Date: 1999-10-29 Impact factor: 17.367
Authors: F Kyndt; V Probst; F Potet; S Demolombe; J C Chevallier; I Baro; J P Moisan; P Boisseau; J J Schott; D Escande; H Le Marec Journal: Circulation Date: 2001-12-18 Impact factor: 29.690
Authors: S G Priori; C Napolitano; M Gasparini; C Pappone; P Della Bella; M Brignole; U Giordano; T Giovannini; C Menozzi; R Bloise; L Crotti; L Terreni; P J Schwartz Journal: Circulation Date: 2000-11-14 Impact factor: 29.690
Authors: Rou-Mu Hu; David J Tester; Ryan Li; Tianyu Sun; Blaise Z Peterson; Michael J Ackerman; Jonathan C Makielski; Bi-Hua Tan Journal: Channels (Austin) Date: 2018 Impact factor: 2.581
Authors: Laura Andreasen; Jonas B Nielsen; Stine Darkner; Ingrid E Christophersen; Javad Jabbari; Lena Refsgaard; Jens J Thiis; Ahmad Sajadieh; Arnljot Tveit; Stig Haunsø; Jesper H Svendsen; Nicole Schmitt; Morten S Olesen Journal: Eur J Hum Genet Date: 2014-03-26 Impact factor: 4.246