Polygenic Risk Score predicts QTc-prolongation and Short-Term Mortality in Patients using QT-prolonging Psychoactive Medications

medRxiv - Genetic and Genomic Medicine Pub Date : 2024-07-25 DOI:10.1101/2024.07.24.24310940

Mays Altaraihi

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Abstract

Background: There is a genetic component to the QT-interval. This study investigated whether a polygenic risk score for QTc (PRSQTc) could predict ∆QTc and short-term mortality in first-time users of QT-prolonging medications (QTPM) with a known risk of Torsade de Pointes. Methods: First-time users of psychoactive QTPM in the Copenhagen Hospital Biobank and the Danish Blood Donor Study from 2009-2021 were included. ∆QTc was calculated and all-cause 30-day mortality following initiation of treatment was explored. All models were adjusted for conventional QT-prolonging risk factors, and models investigating death were additionally adjusted for potential comorbidity confounders. Results: The PRSQTc could predict ∆QTc (2.88 milliseconds (ms) for every increase of standard deviation in PRSQTc (P <0.001)) following treatment initiation. Individuals in the top ≥80 % of PRSQTc had a higher risk of ∆QTc of ≥60 ms compared to individuals in <80 % PRSQTc (OR = 4.88 P = 0.019). Furthermore, the study has also shown that the shorter QTc before initiation of QTPM, the higher the risk of greater ∆QTc. A high PRSQTc could also predict short-term mortality following treatment initiation: Individuals in the top PRSQTc ≥90 % had an odds ratio of 1.84 (P-value = 0.002) for short-term mortality compared to individuals with PRSQTc <90 %. Individuals in the top PRSQTc ≥99 % had an odds ratio of 4.95 (P-value = 0.009) for short-term mortality compared to individuals in the <99 % PRSQTc It could be replicated that PRSQTc ≥90 % was a predictor of short-term mortality with OR 1.52 (P-value = 0.002) compared to PRSQTc <90 % in a bigger cohort (N=15.249). Conclusion: PRSQTc seems to be predictive of ∆QTc following initiation of treatment. PRSQTc proves to be a sufficient predictor of 30-day mortality after initiation of QT-prolonging psychoactive drugs with a known risk of Torsade de Pointes. If used in a clinical setting, PRSQT may help prevent sudden cardiac deaths associated with QTPM.

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多基因风险评分可预测 QTc 延长和使用 QT 延长精神活性药物患者的短期死亡率

背景：QT间期存在遗传因素。本研究调查了 QTc 多基因风险评分（PRSQTc）是否能预测已知有发生 Torsade de Pointes 风险的 QT 延长药物（QTPM）首次使用者的 ∆QTc 和短期死亡率。方法：纳入哥本哈根医院生物库和丹麦献血者研究（2009-2021 年）中首次使用精神活性 QTPM 的人群。∆计算了ΔQTc，并探讨了开始治疗后 30 天的全因死亡率。所有模型都根据传统的 QT 延长风险因素进行了调整，调查死亡的模型还根据潜在的合并症混杂因素进行了调整。结果：PRSQTc 可以预测开始治疗后的ΔQTc（PRSQTc 标准差每增加 2.88 毫秒（P <0.001））。与 PRSQTc 在 <80 % 的人相比，PRSQTc 在前 ≥80 % 的人发生 ∆QTc ≥60 毫秒的风险更高（OR = 4.88 P = 0.019）。此外，研究还表明，QTPM 开始前 QTc 越短，∆QTc 越大的风险越高。高 PRSQTc 还可预测开始治疗后的短期死亡率：与 PRSQTc <90 % 的个体相比，PRSQTc ≥ 90 % 的个体短期死亡率的几率比为 1.84（P 值 = 0.002）。在一个更大的队列中（N=15249），PRSQTc ≥90%与PRSQTc <90%相比，预测短期死亡率的OR值为1.52（P值=0.002）。结论：PRSQTcPRSQTc似乎可以预测开始治疗后的ΔQTc。事实证明，PRSQTc 可以充分预测开始服用 QT 延长的精神药物后 30 天的死亡率，因为已知这种药物有导致 Torsade de Pointes 的风险。如果在临床环境中使用，PRSQT 可能有助于预防与 QTPM 相关的心脏性猝死。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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medRxiv - Genetic and Genomic Medicine

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