Exploring the Risk of Adverse Drug Events in Combination with antiparkinsonics and antipsychotics - a two-decade real-world pharmacovigilance analysis based on the FAERS database.

IF 4.5 2区医学 Q1 CLINICAL NEUROLOGY

International Journal of Neuropsychopharmacology Pub Date : 2025-05-21 DOI:10.1093/ijnp/pyaf033

Junyi Wang, Sen Lin, Chen Bai, Huimin Zhang, Haoqi Liu, Min Wang, Rongjuan Guo

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引用次数: 0

Abstract

Background: The combination of antiparkinsonics and antipsychotic drugs (AP) can improve the motor and mental symptoms of Parkinson's disease (PD) and reduce the actual burden of chronic disease care. To explore the adverse drug events (ADEs) worthy of attention in this treatment management process, we conducted a real-world pharmacovigilance analysis based on the FDA Adverse Event Reporting System (FAERS) database.

Method: The Standard pharmacotherapy for PD include Levodopa/Carbidopa, Entacapone, Rasagiline, Pramipexole, Ropinirole, Rotigotine, Apomorphine and Amantadine, etc. AP includes Quetiapine, Clozapine and Pimavanserin. We collected the ADEs reports of FAERS that conformed to the combination regimens of anti-Parkinson's drugs and AP during the 20-year period from the third quarter of 2004 to the second quarter of 2024. Disproportionate analysis and subgroup analysis were conducted through five algorithms, namely Ω shrinkage measure, additive model, multiplicative model, Combination risk ratio, and Chi-square. The Time to onset (TTO) analysis was used to predict the variation of the risk size of ADEs occurrence over time. Finally, we explored the correlation between population characteristics and the occurrence of ADEs through Logistic regression.

Result: We collected a total of 6,297 cases, including 38,316 ADEs records. The results of the disproportionate analysis show that The ADEs with the highest occurrence frequency include hallucination, general physical health deterioration, somnolence, stoma site discharge, urinary tract infection and memory impairment, etc. The TTO analysis results showed that the median TTO for all ADEs was 657.50 days, the median TTO for infection and inflammation was 716.00 days, and the median TTO for psychiatric symptoms was 823.00 days. All median TTOs conform to the early failure curve. The results of Logistic regression showed that gender was correlated with the occurrence of infection and inflammation, and the female population was more inclined to have IME related to infection and inflammation.

Conclusion: During the combined application of antiparkinsonics and AP, in addition to ADEs such as movement disorders and emerging mental symptoms, the risks of infection and inflammation should also be given key attention. Long-term follow-up should run through the entire process of disease diagnosis and treatment, and attention should be paid to the influence of drug dosage forms and dosages. The medication plan should be adjusted in a timely manner when ADEs occur.

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探索与抗帕金森药和抗精神病药联合使用的药物不良事件的风险-基于FAERS数据库的二十年现实世界药物警戒分析。

背景：抗帕金森药物联合抗精神病药物（AP）可改善帕金森病（PD）的运动和精神症状，减轻慢性病护理的实际负担。为了探讨该治疗管理过程中值得关注的药物不良事件（ADEs），我们基于FDA不良事件报告系统（FAERS）数据库进行了现实世界的药物警戒分析。方法：PD的标准药物治疗包括左旋多巴/卡比多巴、恩他卡彭、雷沙吉兰、普拉克索、罗匹尼罗、罗替戈汀、阿波啡、金刚烷胺等。AP包括喹硫平、氯氮平和匹马万色林。我们收集了2004年第三季度至2024年第二季度20年间符合抗帕金森药物和AP联合方案的FAERS的ADEs报告。通过Ω收缩测度、加性模型、乘性模型、组合风险比、卡方五种算法进行不成比例分析和亚组分析。发作时间（TTO）分析用于预测ade发生的风险大小随时间的变化。最后，我们通过Logistic回归探讨了人群特征与ade发生的相关性。结果：共收集6297例，其中ade记录38316例。不成比例分析结果显示，发生率最高的不良事件包括幻觉、一般身体健康状况恶化、嗜睡、造口部位分泌物、尿路感染和记忆障碍等。TTO分析结果显示，所有不良事件的中位TTO为657.50天，感染和炎症的中位TTO为716.00天，精神症状的中位TTO为823.00天。所有中位tto均符合早期失效曲线。Logistic回归结果显示，性别与感染和炎症的发生相关，女性人群更倾向于发生与感染和炎症相关的IME。结论：抗帕金森药与AP联合应用时，除了运动障碍和新出现的精神症状等不良事件外，还应重点关注感染和炎症的风险。长期随访应贯穿疾病诊疗全过程，并注意药物剂型和剂量的影响。发生不良反应时应及时调整用药计划。

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来源期刊

International Journal of Neuropsychopharmacology 医学-精神病学

CiteScore

8.40

自引率

2.10%

发文量

230

审稿时长

4-8 weeks

期刊介绍： The central focus of the journal is on research that advances understanding of existing and new neuropsychopharmacological agents including their mode of action and clinical application or provides insights into the biological basis of psychiatric disorders and thereby advances their pharmacological treatment. Such research may derive from the full spectrum of biological and psychological fields of inquiry encompassing classical and novel techniques in neuropsychopharmacology as well as strategies such as neuroimaging, genetics, psychoneuroendocrinology and neuropsychology.