Factors associated with drug-drug interactions involving citalopram in the UK Biobank.

IF 3.5 3区 医学 Q1 PSYCHIATRY
Benjamin Laplace, Win Lee Edwin Wong, Marco Menchetti, Diana De Ronchi, Paolo Fusar-Poli, Giuseppe Fanelli, Alessandro Serretti, Cathryn M Lewis, Chiara Fabbri
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引用次数: 0

Abstract

Background: Adults with mood and/or anxiety disorders have increased risks of comorbidities, chronic treatments and polypharmacy, increasing the risk of drug-drug interactions (DDIs) with antidepressants.

Aims: To use primary care records from the UK Biobank to assess DDIs with citalopram, the most widely prescribed antidepressant in UK primary care.

Method: We classified drugs with pharmacokinetic or pharmacodynamic DDIs with citalopram, then identified prescription windows for these drugs that overlapped with citalopram prescriptions in UK Biobank participants with primary care records. We tested for associations of DDI status (yes/no) with sociodemographic and clinical characteristics and with cytochrome 2C19 activity, using univariate tests, then fitted multivariable models for variables that reached Bonferroni-corrected significance.

Results: In UK Biobank primary care data, 25 508 participants received citalopram prescription(s), among which 11 941 (46.8%) had at least one DDI, with an average of 1.96 interacting drugs. The drugs most commonly involved were proton pump inhibitors (40% of co-prescription instances). Individuals with DDIs were more often female and older, had more severe and less treatment-responsive depression, and had higher rates of psychiatric and physical disorders. In the multivariable models, treatment resistance and markers of severity (e.g. history of suicidal and self-harm behaviours) were strongly associated with DDIs, as well as comorbidity with cardiovascular disorders. Cytochrome 2C19 activity was not associated with the occurrence of DDIs.

Conclusions: The high frequency of DDIs with citalopram in fragile groups confirms the need for careful consideration before prescribing and periodic re-evaluation.

英国生物银行中涉及西酞普兰的药物相互作用相关因素。
背景:患有情绪和/或焦虑症的成年人患合并症、慢性治疗和多种药物的风险增加,增加了与抗抑郁药发生药物相互作用(ddi)的风险。目的:利用英国生物银行的初级保健记录来评估西酞普兰的ddi,西酞普兰是英国初级保健中最广泛使用的抗抑郁药。方法:我们将药代动力学或药效学ddi与西酞普兰的药物进行分类,然后在英国生物银行有初级保健记录的参与者中确定这些药物的处方窗口与西酞普兰处方重叠。我们使用单变量检验检验DDI状态(是/否)与社会人口学和临床特征以及细胞色素2C19活性的关联,然后对达到bonferroni校正显著性的变量拟合多变量模型。结果:在UK Biobank初级保健数据中,25 508名参与者接受了西酞普兰处方,其中11 941名(46.8%)至少有一种DDI,平均有1.96种相互作用药物。最常见的药物是质子泵抑制剂(占共处方病例的40%)。患有ddi的个体通常是女性和老年人,患有更严重的抑郁症,治疗反应更差,精神和身体疾病的发病率更高。在多变量模型中,治疗耐药性和严重程度标记(如自杀和自残行为史)与ddi以及心血管疾病的合并症密切相关。细胞色素2C19活性与ddi的发生无关。结论:在脆弱人群中,西酞普兰的ddi频率较高,这证实了在处方前需要仔细考虑并定期重新评估。
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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来源期刊
BJPsych Open
BJPsych Open Medicine-Psychiatry and Mental Health
CiteScore
6.30
自引率
3.70%
发文量
610
审稿时长
16 weeks
期刊介绍: Announcing the launch of BJPsych Open, an exciting new open access online journal for the publication of all methodologically sound research in all fields of psychiatry and disciplines related to mental health. BJPsych Open will maintain the highest scientific, peer review, and ethical standards of the BJPsych, ensure rapid publication for authors whilst sharing research with no cost to the reader in the spirit of maximising dissemination and public engagement. Cascade submission from BJPsych to BJPsych Open is a new option for authors whose first priority is rapid online publication with the prestigious BJPsych brand. Authors will also retain copyright to their works under a creative commons license.
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