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台湾地区患有甲基苯丙胺相关障碍的个体患心肌病风险增加。

Increased risk of cardiomyopathy in individuals with methamphetamine related disorders in Taiwan.

作者信息

Yu Pi-Ching, Hsin Ho-Tsung, Lin Wei-Ting, Huang Yao-Ching, Huang Shi-Hao, Weng Tsu-Hsuan, Wang Bing-Long, Chung Chi-Hsiang, Fann Li-Yun, Chien Wu-Chien, Yang Sung-Sen

机构信息

Graduate Institute of Medicine, National Defense Medical Center, Taipei, 11490, Taiwan.

Cardiovascular Intensive Care Unit, Department of Critical Care Medicine, Far-Eastern Memorial Hospital, New Taipei City, 10602, Taiwan.

出版信息

Sci Rep. 2025 Apr 3;15(1):11449. doi: 10.1038/s41598-025-94591-0.

Abstract

To explore whether Methamphetamine-related disorders (MRDs) will cause the risk of cardiomyopathy in the future. This study used Taiwan's Longitudinal Generation Tracking Database (LGTD) to conduct a 1:4 paired analysis of sex, age, and inclusion year. 17,071 patients with MRDs and 153 patients with cardiomyopathy were selected; 68,264 patients without MRDs and 274 patients with cardiomyopathy were also selected. This study used SPSS 22 statistical software to conduct Cox regression analysis. Patients with MRDs had a 3.421-folds higher risk of cardiomyopathy than patients without MRDs. Men have a 0.735-fold lower risk of developing cardiomyopathy than women. In terms of age group, aged 50-64 and ≧ 65 have a 1.145- and 1.332-folds higher risk of cardiomyopathy, respectively, compared to those aged 20-49. For each one-point increase in Charlson Comorbidity Index (CCI), the risk of cardiomyopathy rises by 58.3%. Specifically, for three types of Methamphetamines (Methamphetamine and other psychostimulant dependence, Methamphetamine or related acting sympathomimetic abuse, Methamphetamine psychosis), the HR for cardiomyopathy in patients with MRDs was 3.864 (p < 0.001), 2.916 (p < 0.001), and 2.295 (p = 0.016) times higher, respectively, compared to patients without MRDs. The Kaplan-Meier log-rank test was used to calculate the cumulative risk of MRDs, showing a significant difference in the cumulative cardiomyopathy incidence between the MRDs and non-MRDs groups (long-rank test, p < 0.001). MRDs will increase the risk of cardiomyopathy. Women are more susceptible to cardiomyopathy than men, and the risk escalates for individuals aged 50-64 and those 65 years or older, compared to the 20-49-year age group. Additionally, an increase in the CCI correlates with a heightened risk of cardiomyopathy. There are important differences between these groups in terms of duration, frequency, and severity of use, with longer exposure and more frequent use increasing the risk of dependence and psychosis, but individual susceptibility, dose, and use patterns also play key roles.

摘要

为探究甲基苯丙胺相关障碍(MRDs)未来是否会导致心肌病风险。本研究利用台湾纵向世代追踪数据库(LGTD),按性别、年龄和纳入年份进行1:4配对分析。选取了17071例患有MRDs的患者和153例患有心肌病的患者;还选取了68264例未患有MRDs的患者和274例患有心肌病的患者。本研究使用SPSS 22统计软件进行Cox回归分析。患有MRDs的患者患心肌病的风险比未患有MRDs的患者高3.421倍。男性患心肌病的风险比女性低0.735倍。在年龄组方面,与20 - 49岁的人群相比,50 - 64岁和≥65岁的人群患心肌病的风险分别高1.145倍和1.332倍。查尔森合并症指数(CCI)每增加1分,患心肌病的风险上升58.3%。具体而言,对于三种类型的甲基苯丙胺(甲基苯丙胺及其他精神兴奋药依赖、甲基苯丙胺或相关拟交感神经兴奋药滥用、甲基苯丙胺所致精神病),患有MRDs的患者患心肌病的风险比未患有MRDs的患者分别高3.864倍(p<0.001)、2.916倍(p<0.001)和2.295倍(p = 0.016)。采用Kaplan - Meier对数秩检验计算MRDs的累积风险,结果显示MRDs组和非MRDs组之间心肌病累积发病率存在显著差异(对数秩检验,p<0.001)。MRDs会增加患心肌病的风险。女性比男性更容易患心肌病,与20 - 年龄组相比,50 - 64岁以及65岁及以上的个体患心肌病的风险更高。此外,CCI的增加与患心肌病风险的升高相关。这些组在使用的持续时间、频率和严重程度方面存在重要差异,接触时间越长、使用频率越高,依赖和精神病的风险就越高,但个体易感性、剂量和使用模式也起着关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bac0/11968872/1ba31aa1be1f/41598_2025_94591_Fig1_HTML.jpg

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