Table2_A mild phenotype associated with KCNQ1 p.V205M mediated long QT syndrome in First Nations children of Northern British Columbia: effect of additional variants and considerations for management.docx

Introduction Congenital Long QT Syndrome (LQTS) is common in a First Nations community in Northern British Columbia due to the founder variant KCNQ1 p.V205M. Although well characterized molecularly and clinically in adults, no data have been previously reported on the pediatric population. The pheno...

Full description

Bibliographic Details
Main Authors: Simona Bene Watts, Barbara Gauthier, Anders C. Erickson, Julie Morrison, Mavis Sebastian, Lawrence Gillman, Sarah McIntosh, Connie Ens, Elizabeth Sherwin, Rod McCormick, Shubhayan Sanatani, Laura Arbour
Format: Dataset
Language:unknown
Published: 2024
Subjects:
Foetal Development and Medicine
Obstetrics and Gynaecology
Paediatrics
Paediatrics and Reproductive Medicine not elsewhere classified
long QT syndrome (LQTS)
First Nations
Indigenous
carnitine palmitoyltransferase 1A
long QT syndrome type 1
KCNQ1
Online Access:https://doi.org/10.3389/fped.2024.1394105.s004
https://figshare.com/articles/dataset/Table2_A_mild_phenotype_associated_with_KCNQ1_p_V205M_mediated_long_QT_syndrome_in_First_Nations_children_of_Northern_British_Columbia_effect_of_additional_variants_and_considerations_for_management_docx/25940572
id ftfrontimediafig:oai:figshare.com:article/25940572
record_format openpolar
spelling ftfrontimediafig:oai:figshare.com:article/25940572 2024-09-15T18:06:32+00:00 Table2_A mild phenotype associated with KCNQ1 p.V205M mediated long QT syndrome in First Nations children of Northern British Columbia: effect of additional variants and considerations for management.docx Simona Bene Watts Barbara Gauthier Anders C. Erickson Julie Morrison Mavis Sebastian Lawrence Gillman Sarah McIntosh Connie Ens Elizabeth Sherwin Rod McCormick Shubhayan Sanatani Laura Arbour 2024-05-31T04:12:01Z https://doi.org/10.3389/fped.2024.1394105.s004 https://figshare.com/articles/dataset/Table2_A_mild_phenotype_associated_with_KCNQ1_p_V205M_mediated_long_QT_syndrome_in_First_Nations_children_of_Northern_British_Columbia_effect_of_additional_variants_and_considerations_for_management_docx/25940572 unknown doi:10.3389/fped.2024.1394105.s004 https://figshare.com/articles/dataset/Table2_A_mild_phenotype_associated_with_KCNQ1_p_V205M_mediated_long_QT_syndrome_in_First_Nations_children_of_Northern_British_Columbia_effect_of_additional_variants_and_considerations_for_management_docx/25940572 CC BY 4.0 Foetal Development and Medicine Obstetrics and Gynaecology Paediatrics Paediatrics and Reproductive Medicine not elsewhere classified long QT syndrome (LQTS) First Nations Indigenous carnitine palmitoyltransferase 1A long QT syndrome type 1 KCNQ1 Dataset 2024 ftfrontimediafig https://doi.org/10.3389/fped.2024.1394105.s004 2024-08-19T06:19:45Z Introduction Congenital Long QT Syndrome (LQTS) is common in a First Nations community in Northern British Columbia due to the founder variant KCNQ1 p.V205M. Although well characterized molecularly and clinically in adults, no data have been previously reported on the pediatric population. The phenotype in adults has been shown to be modified by a splice site variant in KCNQ1 (p.L353L). The CPT1A p.P479L metabolic variant, also common in Northern Indigenous populations, is associated with hypoglycemia and infant death. Since hypoglycemia can affect the corrected QT interval (QTc) and may confer risk for seizures (also associated with LQTS), we sought to determine the effect of all three variants on the LQTS phenotype in children within our First Nations cohort. Methods As part of a larger study assessing those with LQTS and their relatives in a Northern BC First Nation, we assessed those entering the study from birth to age 18 years. We compared the corrected peak QTc and potential cardiac events (syncope/seizures) of 186 children from birth to 18 years, with and without the KCNQ1 (p.V205M and p.L353L) and CPT1A variants, alone and in combination. Linear and logistic regression and student t-tests were applied as appropriate. Results Only the KCNQ1 p.V205M variant conferred a significant increase in peak QTc 23.8 ms (p < 0.001) above baseline, with females increased by 30.1 ms (p < 0.001) and males by 18.9 ms (p < 0.01). There was no evidence of interaction effects with the other two variants studied. Although the p.V205M variant was not significantly associated with syncope/seizures, the odds of having a seizure/syncope were significantly increased for those homozygous for CPT1A p.P479L compared to homozygous wild type (Odds Ratio [OR]3.0 [95% confidence interval (CI) 1.2–7.7]; p = 0.019). Conclusion While the KCNQ1 p.V205M variant prolongs the peak QTc, especially in females, the CPT1A p.P479L variant is more strongly associated with loss of consciousness events. These findings suggest that effect of ... Dataset First Nations Frontiers: Figshare
institution Open Polar
collection Frontiers: Figshare
op_collection_id ftfrontimediafig
language unknown
topic Foetal Development and Medicine
Obstetrics and Gynaecology
Paediatrics
Paediatrics and Reproductive Medicine not elsewhere classified
long QT syndrome (LQTS)
First Nations
Indigenous
carnitine palmitoyltransferase 1A
long QT syndrome type 1
KCNQ1
spellingShingle Foetal Development and Medicine
Obstetrics and Gynaecology
Paediatrics
Paediatrics and Reproductive Medicine not elsewhere classified
long QT syndrome (LQTS)
First Nations
Indigenous
carnitine palmitoyltransferase 1A
long QT syndrome type 1
KCNQ1
Simona Bene Watts
Barbara Gauthier
Anders C. Erickson
Julie Morrison
Mavis Sebastian
Lawrence Gillman
Sarah McIntosh
Connie Ens
Elizabeth Sherwin
Rod McCormick
Shubhayan Sanatani
Laura Arbour
Table2_A mild phenotype associated with KCNQ1 p.V205M mediated long QT syndrome in First Nations children of Northern British Columbia: effect of additional variants and considerations for management.docx
topic_facet Foetal Development and Medicine
Obstetrics and Gynaecology
Paediatrics
Paediatrics and Reproductive Medicine not elsewhere classified
long QT syndrome (LQTS)
First Nations
Indigenous
carnitine palmitoyltransferase 1A
long QT syndrome type 1
KCNQ1
description Introduction Congenital Long QT Syndrome (LQTS) is common in a First Nations community in Northern British Columbia due to the founder variant KCNQ1 p.V205M. Although well characterized molecularly and clinically in adults, no data have been previously reported on the pediatric population. The phenotype in adults has been shown to be modified by a splice site variant in KCNQ1 (p.L353L). The CPT1A p.P479L metabolic variant, also common in Northern Indigenous populations, is associated with hypoglycemia and infant death. Since hypoglycemia can affect the corrected QT interval (QTc) and may confer risk for seizures (also associated with LQTS), we sought to determine the effect of all three variants on the LQTS phenotype in children within our First Nations cohort. Methods As part of a larger study assessing those with LQTS and their relatives in a Northern BC First Nation, we assessed those entering the study from birth to age 18 years. We compared the corrected peak QTc and potential cardiac events (syncope/seizures) of 186 children from birth to 18 years, with and without the KCNQ1 (p.V205M and p.L353L) and CPT1A variants, alone and in combination. Linear and logistic regression and student t-tests were applied as appropriate. Results Only the KCNQ1 p.V205M variant conferred a significant increase in peak QTc 23.8 ms (p < 0.001) above baseline, with females increased by 30.1 ms (p < 0.001) and males by 18.9 ms (p < 0.01). There was no evidence of interaction effects with the other two variants studied. Although the p.V205M variant was not significantly associated with syncope/seizures, the odds of having a seizure/syncope were significantly increased for those homozygous for CPT1A p.P479L compared to homozygous wild type (Odds Ratio [OR]3.0 [95% confidence interval (CI) 1.2–7.7]; p = 0.019). Conclusion While the KCNQ1 p.V205M variant prolongs the peak QTc, especially in females, the CPT1A p.P479L variant is more strongly associated with loss of consciousness events. These findings suggest that effect of ...
format Dataset
author Simona Bene Watts
Barbara Gauthier
Anders C. Erickson
Julie Morrison
Mavis Sebastian
Lawrence Gillman
Sarah McIntosh
Connie Ens
Elizabeth Sherwin
Rod McCormick
Shubhayan Sanatani
Laura Arbour
author_facet Simona Bene Watts
Barbara Gauthier
Anders C. Erickson
Julie Morrison
Mavis Sebastian
Lawrence Gillman
Sarah McIntosh
Connie Ens
Elizabeth Sherwin
Rod McCormick
Shubhayan Sanatani
Laura Arbour
author_sort Simona Bene Watts
title Table2_A mild phenotype associated with KCNQ1 p.V205M mediated long QT syndrome in First Nations children of Northern British Columbia: effect of additional variants and considerations for management.docx
title_short Table2_A mild phenotype associated with KCNQ1 p.V205M mediated long QT syndrome in First Nations children of Northern British Columbia: effect of additional variants and considerations for management.docx
title_full Table2_A mild phenotype associated with KCNQ1 p.V205M mediated long QT syndrome in First Nations children of Northern British Columbia: effect of additional variants and considerations for management.docx
title_fullStr Table2_A mild phenotype associated with KCNQ1 p.V205M mediated long QT syndrome in First Nations children of Northern British Columbia: effect of additional variants and considerations for management.docx
title_full_unstemmed Table2_A mild phenotype associated with KCNQ1 p.V205M mediated long QT syndrome in First Nations children of Northern British Columbia: effect of additional variants and considerations for management.docx
title_sort table2_a mild phenotype associated with kcnq1 p.v205m mediated long qt syndrome in first nations children of northern british columbia: effect of additional variants and considerations for management.docx
publishDate 2024
url https://doi.org/10.3389/fped.2024.1394105.s004
https://figshare.com/articles/dataset/Table2_A_mild_phenotype_associated_with_KCNQ1_p_V205M_mediated_long_QT_syndrome_in_First_Nations_children_of_Northern_British_Columbia_effect_of_additional_variants_and_considerations_for_management_docx/25940572
genre First Nations
genre_facet First Nations
op_relation doi:10.3389/fped.2024.1394105.s004
https://figshare.com/articles/dataset/Table2_A_mild_phenotype_associated_with_KCNQ1_p_V205M_mediated_long_QT_syndrome_in_First_Nations_children_of_Northern_British_Columbia_effect_of_additional_variants_and_considerations_for_management_docx/25940572
op_rights CC BY 4.0
op_doi https://doi.org/10.3389/fped.2024.1394105.s004
_version_ 1810443961805832192

Similar Items