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Different Doses of Pharmacological Treatments for Mild to Moderate Alzheimer’s Disease: A Bayesian Network Meta-Analysis

机译:不同剂量的药理治疗,用于轻度至中度阿尔茨海默病:贝叶斯网络元分析

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Pharmacological treatments play a significant role in treating mild to moderate Alzheimer’s disease (AD), but the optimal doses of various drugs used for these treatments are unknown. Our study compared the efficacy, acceptability, and safety of different doses of pharmacological treatments for mild to moderate AD. Methods: Randomized controlled trials (RCTs) were identified by searching the PubMed, EMBASE, and Cochrane Library databases (all RCTs published from the date of inception of the databases until September 19, 2019). Trials comparing the efficacy, acceptability, and safety of pharmacological interventions involving donepezil, galantamine, rivastigmine, memantine, huperzine A, and Ginkgo biloba extract EGb761, alone or in combination, were identified. The primary outcomes were efficacy, acceptability, and safety. Results: Our meta-analysis included 37 studies involving 14,705 participants. In terms of improving cognitive function, galantamine 32 mg, galantamine 24 mg, donepezil 5 mg, and donepezil 10 mg were more effective than other interventions, with the surface under the cumulative ranking curve (SUCRA) values of 93.2, 75.5, 73.3, and 65.6%, respectively. According to the SUCRA values, EGb761 240 mg was considered to be the optimal intervention in terms of both acceptability and safety. With regard to clinical global impression, rivastigmine 12 mg had the highest probability of being ranked first (83.7%). The rivastigmine 15 cm2 patch (SUCRA = 93.7%) may be the best choice for daily living. However, there were no interventions that could significantly improve neuropsychiatric symptoms, compared with the placebo. Conclusions: Different doses of the tested pharmacological interventions yielded benefits with regard to cognition, acceptability, safety, function, and clinical global impressions, but not effective behaviors.
机译:药理治疗在治疗轻度至中度阿尔茨海默病(AD)中发挥着重要作用,但是用于这些治疗的各种药物的最佳剂量是未知的。我们的研究比较了不同剂量药理治疗的疗效,可接受性和安全性,用于轻度至中度广告。方法:通过搜索Pubmed,Embase和Cochrane库数据库来确定随机对照试验(RCT)(从数据库开始于2019年9月19日开始发布的所有RCT)。试验比较涉及Deinpezil,Galantamine,Rivastigmine,Memantine,Huperzine A和Ginkgo Biloba提取EGB761,单独或组合的药理干预的疗效,可接受性和安全性。主要结果是有效性,可接受性和安全性。结果:我们的META分析包括37项涉及14,705名参与者的研究。在改善认知功能方面,加兰汀32mg,加兰汀24mg,Deppezil 5mg,Denpezil 10mg比其他干预更有效,累积排名曲线(Sucra)值为93.2,75.5,73.3和分别为65.6%。根据Sucra值,EGB761 240mg被认为是可接受性和安全性方面的最佳干预。关于临床全球性印象,RIVASTIGMINE 12 MG的概率最高(83.7%)。 Rivastigmine 15 cm2贴片(Sucra = 93.7%)可能是日常生活的最佳选择。然而,与安慰剂相比,没有干预措施可以显着改善神经精神症状。结论:不同剂量的测试药理学干预措施在认知,可接受性,安全性,功能和临床全球印象方面产生了益处,但不能有效的行为。

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