Risk of Major Adverse Cardiovascular Events Following Nicotinamide Exposure.

IF 11 1区 医学 Q1 DERMATOLOGY JAMA dermatology Pub Date : 2025-02-26 DOI:10.1001/jamadermatol.2025.0001
Lee Wheless, Ranya Guennoun, Basia Michalski-McNeely, Katlyn M Gonzalez, Rachel Weiss, Siwei Zhang, Lydia Yao, Chris Madden, Hua-Chang Chen, Jefferson L Triozzi, Ran Tao, Otis Wilson, Quinn S Wells, Adriana Hung, Kristin Bibee, Rebecca I Hartman, Yaomin Xu
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引用次数: 0

Abstract

Importance: Nicotinamide metabolites have recently been implicated in increased risk of major cardiovascular events (MACE). Supportive data about clinical risk of MACE for nicotinamide users is lacking.

Objective: To determine whether nicotinamide use results in an increase of MACE.

Design, setting, and participants: This study used retrospective electronic health record data of 2 patient cohorts, the Vanderbilt University Medical Center (VUMC) and Million Veteran Program (MVP). The risk of MACE in patients exposed to nicotinamide was compared with the risk of MACE in unexposed patients. In the VUMC cohort, patients were either exposed to nicotinamide based on keyword entry for nicotinamide or niacinamide and manual review of medical records or were unexposed but had documented recommendation for use. In the MVP cohort, those exposed to nicotinamide were matched via propensity scores to those who were not exposed. Data were collected from January 1989 to February 2024, and data were analyzed from March to December 2024.

Exposures: The primary exposure for the VUMC cohort was a confirmed exposure to nicotinamide on medical record review. The primary exposure for the MVP cohort was medication entry for nicotinamide or niacinamide.

Main outcomes and measures: The primary outcome was development of MACE based on a validated phenotype.

Results: Of 13 108 included patients, 11 926 (91.0%) were male, and the mean (SD) age was 66.8 (11.5) years. In the VUMC cohort, 1228 patients were exposed to nicotinamide and 253 were unexposed; in the MVP cohort, 4063 were exposed and 7564 were not. A total of 5291 had exposure to nicotinamide. Neither cohort had significant differences in mean age, sex, race, or ethnicity between the nicotinamide exposed and unexposed groups. There was no difference in the cumulative incidence of MACE after nicotinamide exposure in either the VUMC cohort or MVP cohorts. In adjusted cause-specific models stratified by history of prior MACE, there was no significant association between nicotinamide exposure and the primary outcome of MACE in either the VUMC cohort (no prior MACE: hazard ratio [HR], 2.02; 95% CI, 0.81-5.05; prior MACE: HR, 0.46; 95% CI, 0.22-0.95) or MVP cohort (no prior MACE: HR, 1.07; 95% CI, 0.75-1.17; prior MACE: HR, 1.04; 95% CI, 0.53-2.06).

Conclusions and relevance: In this retrospective cohort study of 13 108 adults from 2 different patient populations, there was no increased risk of MACE in patients with nicotinamide exposure.

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接触尼古丁酰胺后发生重大不良心血管事件的风险。
重要性:烟酰胺代谢物最近被认为与主要心血管事件(MACE)的风险增加有关。缺乏烟酰胺使用者MACE临床风险的支持性数据。目的:探讨烟酰胺是否会导致MACE升高。设计、设置和参与者:本研究使用范德比尔特大学医学中心(VUMC)和百万退伍军人计划(MVP)两个患者队列的回顾性电子健康记录数据。将暴露于烟酰胺的患者的MACE风险与未暴露于烟酰胺的患者的MACE风险进行比较。在VUMC队列中,患者要么根据烟酰胺或烟酰胺的关键字输入和医疗记录的人工审查暴露于烟酰胺,要么未暴露于烟酰胺,但有书面推荐使用。在MVP队列中,那些暴露于烟酰胺的人通过倾向得分与那些没有暴露的人相匹配。数据采集时间为1989年1月至2024年2月,分析时间为2024年3月至12月。暴露:VUMC队列的主要暴露是经医疗记录审查确认的烟酰胺暴露。MVP队列的主要暴露是烟酰胺或烟酰胺的药物进入。主要结局和测量:主要结局是基于验证表型的MACE发展。结果:13 108例纳入的患者中,男性11 926例(91.0%),平均(SD)年龄66.8(11.5)岁。在VUMC队列中,1228名患者暴露于烟酰胺,253名未暴露;在MVP队列中,4063人暴露,7564人未暴露。共有5291人暴露于烟酰胺。在烟酰胺暴露组和未暴露组之间,两个队列在平均年龄、性别、种族或民族方面都没有显著差异。在VUMC队列和MVP队列中,烟酰胺暴露后MACE的累积发生率没有差异。在按既往MACE史分层的调整后的病因特异性模型中,在VUMC队列中,烟酰胺暴露与MACE的主要结局之间均无显著关联(无既往MACE:风险比[HR], 2.02;95% ci, 0.81-5.05;先前MACE: HR, 0.46;95% CI, 0.22-0.95)或MVP队列(无既往MACE: HR, 1.07;95% ci, 0.75-1.17;既往MACE: HR, 1.04;95% ci, 0.53-2.06)。结论和相关性:在这项来自2个不同患者群体的13 108名成年人的回顾性队列研究中,烟酰胺暴露患者的MACE风险没有增加。
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来源期刊
JAMA dermatology
JAMA dermatology DERMATOLOGY-
CiteScore
14.10
自引率
5.50%
发文量
300
期刊介绍: JAMA Dermatology is an international peer-reviewed journal that has been in continuous publication since 1882. It began publication by the American Medical Association in 1920 as Archives of Dermatology and Syphilology. The journal publishes material that helps in the development and testing of the effectiveness of diagnosis and treatment in medical and surgical dermatology, pediatric and geriatric dermatology, and oncologic and aesthetic dermatologic surgery. JAMA Dermatology is a member of the JAMA Network, a consortium of peer-reviewed, general medical and specialty publications. It is published online weekly, every Wednesday, and in 12 print/online issues a year. The mission of the journal is to elevate the art and science of health and diseases of skin, hair, nails, and mucous membranes, and their treatment, with the aim of enabling dermatologists to deliver evidence-based, high-value medical and surgical dermatologic care. The journal publishes a broad range of innovative studies and trials that shift research and clinical practice paradigms, expand the understanding of the burden of dermatologic diseases and key outcomes, improve the practice of dermatology, and ensure equitable care to all patients. It also features research and opinion examining ethical, moral, socioeconomic, educational, and political issues relevant to dermatologists, aiming to enable ongoing improvement to the workforce, scope of practice, and the training of future dermatologists. JAMA Dermatology aims to be a leader in developing initiatives to improve diversity, equity, and inclusion within the specialty and within dermatology medical publishing.
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