The Contribution of Known Familial Cardiovascular Disease Genes to Sudden Cardiac Death in Patients Undergoing Hemodialysis.

Tae-Hwi Schwantes-An Matteo Vatta Marco Abreu Leah Wetherill Howard J Edenberg Tatiana M Foroud Glenn M Chertow Sharon M Moe

Cardiorenal Med

Division of Nephrology and Hypertension, Department of Medicine, Indiana University School of Medicine, Indianapolis, Indiana, USA.

Published: October 2021

Patients with chronic kidney disease are at high risk for cardiovascular problems, particularly sudden cardiac death (SCD), which is a significant cause of mortality during dialysis.
A study compared 126 SCD patients with 107 controls to explore the link between rare genetic variants associated with cardiovascular death and SCD in those on hemodialysis.
Results indicated no significant genetic associations, suggesting that genetics may not play a major role in SCD for patients undergoing hemodialysis, despite examining 174 relevant genes.

Introduction: Patients with chronic kidney disease experience high rates of cardiovascular mortality and morbidity. When kidney disease progresses to the need for dialysis, sudden cardiac death (SCD) accounts for 25-35% of all cardiovascular deaths. The objective was to determine if rare genetic variants known to be associated with cardiovascular death in the general population are associated with SCD in patients undergoing hemodialysis.

Methods: We performed a case-control study comparing 126 (37 African American [AfAn] and 89 European ancestry [EA]) SCD subjects and 107 controls (34 AfAn and 73 EA), matched for age, sex, self-reported race, dialysis duration (<2, 2-5 and >5 years), and the presence or absence of diabetes mellitus. To target the coding regions of genes previously reported to be associated with 15 inherited cardiac conditions (ICCs), we used the TruSight Cardio Kit (Illumina, San Diego, CA, USA) to capture the genetic regions of interest. In all, the kit targets 572-kb regions that include the protein-coding regions and 40-bp 5' and 3' end-flanking regions of 174 genes associated with the 15 ICCs. Using the sequence data, burden tests were conducted to identify genes with an increased number of variants among SCD cases compared to matched controls.

Results: Eleven genes were associated with SCD, but after correction for multiple testing, none of the 174 genes were identified as having more variants in the SCD cases than the matched controls, including previously identified genes. Secondary burden tests grouping variants based on diseases and gene function did not produce statistically significant associations.

Discussion/conclusions: We found no associations between genes known to be associated with ICCs and SCD in our sample of patients undergoing hemodialysis. This suggests that genetic causes are unlikely to be a major pathogenic factor in SCD in hemodialysis patients, although our sample size limits definitive conclusions.

Download full-text PDF	Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8393692	PMC
http://dx.doi.org/10.1159/000517123	DOI Listing

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