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Loss-of-Function KCNE2 Variants: True Monogenic Culprits of Long-QT Syndrome or Proarrhythmic Variants Requiring Secondary Provocation?
Roberts, Jason D; Krahn, Andrew D; Ackerman, Michael J; Rohatgi, Ram K; Moss, Arthur J; Nazer, Babak; Tadros, Rafik; Gerull, Brenda; Sanatani, Shubhayan; Wijeyeratne, Yanushi D; Baruteau, Alban-Elouen; Muir, Alison R; Pang, Benjamin; Cadrin-Tourigny, Julia; Talajic, Mario; Rivard, Lena; Tester, David J; Liu, Taylor; Whitman, Isaac R; Wojciak, Julianne; Conacher, Susan; Gula, Lorne J; Leong-Sit, Peter; Manlucu, Jaimie; Green, Martin S; Hamilton, Robert; Healey, Jeff S; Lopes, Coeli M; Behr, Elijah R; Wilde, Arthur A; Gollob, Michael H; Scheinman, Melvin M.
Affiliation
  • Roberts JD; For author affiliations, please see the Appendix. jason.roberts@lhsc.on.ca.
  • Krahn AD; For author affiliations, please see the Appendix.
  • Ackerman MJ; For author affiliations, please see the Appendix.
  • Rohatgi RK; For author affiliations, please see the Appendix.
  • Moss AJ; For author affiliations, please see the Appendix.
  • Nazer B; For author affiliations, please see the Appendix.
  • Tadros R; For author affiliations, please see the Appendix.
  • Gerull B; For author affiliations, please see the Appendix.
  • Sanatani S; For author affiliations, please see the Appendix.
  • Wijeyeratne YD; For author affiliations, please see the Appendix.
  • Baruteau AE; For author affiliations, please see the Appendix.
  • Muir AR; For author affiliations, please see the Appendix.
  • Pang B; For author affiliations, please see the Appendix.
  • Cadrin-Tourigny J; For author affiliations, please see the Appendix.
  • Talajic M; For author affiliations, please see the Appendix.
  • Rivard L; For author affiliations, please see the Appendix.
  • Tester DJ; For author affiliations, please see the Appendix.
  • Liu T; For author affiliations, please see the Appendix.
  • Whitman IR; For author affiliations, please see the Appendix.
  • Wojciak J; For author affiliations, please see the Appendix.
  • Conacher S; For author affiliations, please see the Appendix.
  • Gula LJ; For author affiliations, please see the Appendix.
  • Leong-Sit P; For author affiliations, please see the Appendix.
  • Manlucu J; For author affiliations, please see the Appendix.
  • Green MS; For author affiliations, please see the Appendix.
  • Hamilton R; For author affiliations, please see the Appendix.
  • Healey JS; For author affiliations, please see the Appendix.
  • Lopes CM; For author affiliations, please see the Appendix.
  • Behr ER; For author affiliations, please see the Appendix.
  • Wilde AA; For author affiliations, please see the Appendix.
  • Gollob MH; For author affiliations, please see the Appendix.
  • Scheinman MM; For author affiliations, please see the Appendix.
Circ Arrhythm Electrophysiol ; 10(8)2017 Aug.
Article in En | MEDLINE | ID: mdl-28794082
ABSTRACT

BACKGROUND:

Insight into type 6 long-QT syndrome (LQT6), stemming from mutations in the KCNE2-encoded voltage-gated channel ß-subunit, is limited. We sought to further characterize its clinical phenotype. METHODS AND

RESULTS:

Individuals with reported pathogenic KCNE2 mutations identified during arrhythmia evaluation were collected from inherited arrhythmia clinics and the Rochester long-QT syndrome (LQTS) registry. Previously reported LQT6 cases were identified through a search of the MEDLINE database. Clinical features were assessed, while reported KCNE2 mutations were evaluated for genotype-phenotype segregation and classified according to the contemporary American College of Medical Genetics guidelines. Twenty-seven probands possessed reported pathogenic KCNE2 mutations, while a MEDLINE search identified 17 additional LQT6 cases providing clinical and genetic data. Sixteen probands had normal resting QTc values and only developed QT prolongation and malignant arrhythmias after exposure to QT-prolonging stressors, 10 had other LQTS pathogenic mutations, and 10 did not have an LQTS phenotype. Although the remaining 8 subjects had an LQTS phenotype, evidence suggested that the KCNE2 variant was not the underlying culprit. The collective frequency of KCNE2 variants implicated in LQT6 in the Exome Aggregation Consortium database was 1.4%, in comparison with a 0.0005% estimated clinical prevalence for LQT6.

CONCLUSIONS:

On the basis of clinical phenotype, the high allelic frequencies of LQT6 mutations in the Exome Aggregation Consortium database, and absence of previous documentation of genotype-phenotype segregation, our findings suggest that many KCNE2 variants, and perhaps all, have been erroneously designated as LQTS-causative mutations. Instead, KCNE2 variants may confer proarrhythmic susceptibility when provoked by additional environmental/acquired or genetic factors, or both.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Long QT Syndrome / Potassium Channels, Voltage-Gated Type of study: Guideline / Prognostic_studies / Risk_factors_studies Limits: Adolescent / Adult / Aged / Aged80 / Child / Child, preschool / Female / Humans / Male / Middle aged Language: En Journal: Circ Arrhythm Electrophysiol Journal subject: ANGIOLOGIA / CARDIOLOGIA Year: 2017 Document type: Article
Fulltext
Add to My VHL
Print
XML
PubMed Links
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Long QT Syndrome / Potassium Channels, Voltage-Gated Type of study: Guideline / Prognostic_studies / Risk_factors_studies Limits: Adolescent / Adult / Aged / Aged80 / Child / Child, preschool / Female / Humans / Male / Middle aged Language: En Journal: Circ Arrhythm Electrophysiol Journal subject: ANGIOLOGIA / CARDIOLOGIA Year: 2017 Document type: Article