Department of Pharmacy & Pharmacology, University of Bath, Bath, UK.
Centre for Therapeutic Innovation, University of Bath, Bath, UK.
Pharmacoepidemiol Drug Saf. 2022 Aug;31(8):883-891. doi: 10.1002/pds.5480. Epub 2022 May 25.
Older adults are at an increased risk of delirium because of age, polypharmacy, multiple comorbidities and acute illness. Antimuscarinics are the backbone of the pharmacological management of overactive bladder. However, the safety profiles of antimuscarinics vary because of their dissimilarities to muscarinic receptor-subtype affinities and are associated with differential central anticholinergic adverse effects.
This study aimed to examine delirium risk in new users of oxybutynin and solifenacin in older adults (≥ 65 years). In the secondary analyses, we examined the risk of delirium by type and dose of antimuscarinic.
We applied a case-time-control design to investigate delirium risk in older adults who started taking oxybutynin and solifenacin. We used a nationwide inpatient hospital data (2005-2016), National Minimum Data Set, maintained by the Ministry of Health, New Zealand (NZ), to identify older adults with a new-onset diagnosis of delirium. Eligible patients were older adults aged 65 at entry into the cohort on 1/1/2006. We used dispensing claims data to determine antimuscarinic treatment exposure. The antimuscarinic included in the study were new users of oxybutynin and solifenacin. These two antimuscarinics are subsidised by the Pharmaceutical Management Agency and are the most frequently used antimuscarinic in NZ. A conditional logistic regression model was used to compute matched odds ratios (MORs) and 95% confidence intervals (CIs). In the case-time-control design, we made separate analyses to evaluate the dose-response risk of delirium.
We identified 4818 individuals (mean age 82.14) from 2005 to 2015 with incident delirium and were exposed to at least one of the antimuscarinic of interest. The case-time-control matched odds ratio (MOR) for delirium with oxybutynin was (2.06, 95% confidence interval [CI] 1.07-3.96). Solifenacin was not associated with delirium (0.89 95%CI 0.64-1.23). In the sensitivity analyses, the case-time-control MOR for delirium using a shorter risk period (0-3 days) did not change the results. The dose-response risk of delirium was significant for oxybutynin (0.05, 95%CI 0.02-0.08) but not for solifenacin (-0.01, 95%CI -0.03 to 0.00). In addition, in the subgroup analyses, a statistically significant association of delirium was found for oxybutynin but not for solifenacin in the non-dementia cohort (2.11,95% CI 1.08-4.13) and the dementia cohort (1.25, 95%CI 0.05-26.9).
The study found that oxybutynin but not solifenacin is associated with a risk of new-onset delirium in older adults. The higher blockade of M1 and M2 receptors by oxybutynin is likely to contribute to delirium than solifenacin, which is highly selective for the M3 receptor subtype. Therefore, the treatment choice with an M3 selective agent must be given due consideration, particularly in those with pre-existing cognitive impairment.
由于年龄、多种药物并用、多种合并症和急性疾病,老年人患谵妄的风险增加。抗毒蕈碱药物是治疗膀胱过度活动症的药物治疗的基础。然而,由于它们与毒蕈碱受体亚型亲和力的不同,抗毒蕈碱药物的安全性特征各不相同,并且与不同的中枢抗胆碱能不良反应相关。
本研究旨在检查新使用奥昔布宁和索利那新的老年人(≥65 岁)发生谵妄的风险。在二次分析中,我们通过抗毒蕈碱药物的类型和剂量来检查谵妄的风险。
我们应用病例时间对照设计来研究新开始使用奥昔布宁和索利那新的老年人发生谵妄的风险。我们使用全国住院医院数据(2005-2016 年)、卫生部维护的新西兰国家最低数据集(Ministry of Health, New Zealand,NZ)来确定新诊断为谵妄的老年人。符合条件的患者是在 2006 年 1 月 1 日进入队列时年龄为 65 岁的老年人。我们使用配药索赔数据来确定抗毒蕈碱药物的治疗暴露情况。纳入研究的抗毒蕈碱药物是新使用奥昔布宁和索利那新的药物。这两种抗毒蕈碱药物均由药品管理局资助,是新西兰最常使用的抗毒蕈碱药物。我们使用条件逻辑回归模型计算匹配比值比(matched odds ratios,MORs)和 95%置信区间(95% confidence intervals,CIs)。在病例时间对照设计中,我们进行了单独的分析,以评估谵妄的剂量反应风险。
我们从 2005 年至 2015 年确定了 4818 名(平均年龄 82.14 岁)有新发谵妄且至少使用过一种感兴趣的抗毒蕈碱药物的患者。奥昔布宁发生谵妄的病例时间对照匹配比值比(matched odds ratio,MOR)为 2.06(95%CI 1.07-3.96)。索利那新与谵妄无关(0.89,95%CI 0.64-1.23)。在敏感性分析中,使用较短风险期(0-3 天)的病例时间对照 MOR 并没有改变结果。奥昔布宁的谵妄剂量反应风险显著(0.05,95%CI 0.02-0.08),但索利那新的风险不显著(-0.01,95%CI-0.03 至 0.00)。此外,在亚组分析中,奥昔布宁与非痴呆队列(2.11,95%CI 1.08-4.13)和痴呆队列(1.25,95%CI 0.05-26.9)中谵妄的发生有统计学显著关联,但索利那新则没有。
本研究发现奥昔布宁而非索利那新与老年人新发谵妄的风险相关。奥昔布宁对 M1 和 M2 受体的更高阻断作用可能比高度选择性 M3 受体亚型的索利那新更容易导致谵妄。因此,必须考虑选择使用 M3 选择性药物,特别是在那些有先前认知障碍的患者中。
