Risk Prediction in Male Adolescents With Congenital Long QT Syndrome: Implications for Sex‐Specific Risk Stratification in Potassium Channel‐Mediated Long QT Syndrome

Author:

Bjelic Milica12ORCID,Goldenberg Ido13ORCID,Younis Arwa14ORCID,Chen Anita Y.5,Huang David T.6ORCID,Yoruk Ayhan7,Aktas Mehmet K.6ORCID,Rosero Spencer6ORCID,Cutter Kristina1,McNitt Scott1ORCID,Sotoodehnia Nona8ORCID,Kudenchuk Peter J.9ORCID,Rea Thomas D.9,Arking Dan E.10ORCID,Zareba Wojciech1ORCID,Ackerman Michael J.11ORCID,Goldenberg Ilan1ORCID

Affiliation:

1. Clinical Cardiovascular Research Center, Division of Cardiology University of Rochester Medical Center Rochester NY USA

2. Department of Anesthesiology St. Elizabeth’s Medical Center Boston University School of Medicine Boston MA USA

3. Department of Medicine, Rochester Regional Health Rochester NY USA

4. Department of Cardiovascular Medicine Cleveland Clinic Cleveland OH USA

5. Department of Biostatistics and Computational Biology University of Rochester Medical Center Rochester NY USA

6. Department of Medicine, Division of Cardiology University of Rochester Medical Center Rochester NY USA

7. Division of Cardiology The University of California, San Francisco Medical Center San Francisco CA USA

8. Department of Medicine, Division of Cardiology University of Washington Seattle WA USA

9. Department of Medicine University of Washington Seattle WA USA

10. The McKusick‐Nathans Institute, Department of Genetic Medicine John Hopkins University School of Medicine Baltimore MD USA

11. Departments of Cardiovascular Medicine, Pediatric and Adolescent Medicine, and Molecular Pharmacology & Experimental Therapeutics, Divisions of Heart Rhythm Services and Pediatric Cardiology, Windland Smith Rice Genetic Heart Rhythm Clinic and Windland Smith Rice Sudden Death Genomics Laboratory Mayo Clinic Rochester MN USA

Abstract

Background Sex‐specific risk management may improve outcomes in congenital long QT syndrome (LQTS). We recently developed a prediction score for cardiac events (CEs) and life‐threatening events (LTEs) in postadolescent women with LQTS. In the present study, we aimed to develop personalized risk estimates for the burden of CEs and LTEs in male adolescents with potassium channel‐mediated LQTS. Methods and Results The prognostic model was derived from the LQTS Registry headquartered in Rochester, NY, comprising 611 LQT1 or LQT2 male adolescents from age 10 through 20 years, using the following variables: genotype/mutation location, QTc‐specific thresholds, history of syncope, and β‐blocker therapy. Anderson‐Gill modeling was performed for the end point of CE burden (total number of syncope, aborted cardiac arrest, and appropriate defibrillator shocks). The applicability of the CE prediction model was tested for the end point of the first LTE (excluding syncope and adding sudden cardiac death) using Cox modeling. A total of 270 CEs occurred during follow‐up. The genotype–phenotype risk prediction model identified low‐, intermediate‐, and high‐risk groups, comprising 74%, 14%, and 12% of the study population, respectively. Compared with the low‐risk group, high‐risk male subjects experienced a pronounced 5.2‐fold increased risk of recurrent CEs ( P <0.001), whereas intermediate‐risk patients had a 2.1‐fold ( P =0.004) increased risk . At age 20 years, the low‐, intermediate‐, and high‐risk adolescent male patients had on average 0.3, 0.6, and 1.4 CEs per person, respectively. Corresponding 10‐year adjusted probabilities for a first LTE were 2%, 6%, and 8%. Conclusions Personalized genotype–phenotype risk estimates can be used to guide sex‐specific management in male adolescents with potassium channel‐mediated LQTS.

Publisher

Ovid Technologies (Wolters Kluwer Health)

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