阿尔茨海默病药物治疗指南- fda批准的药物入门

IF 0.8 Q4 CLINICAL NEUROLOGY
Ashvin Varadharajan, Aarjith Damian Davis, Aishwarya Ghosh, Tejaswini Jagtap, Anjo Xavier, Anjana Jayakumar Menon, Dwaiti Roy, Sandhya Gandhi, Thomas Gregor
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引用次数: 0

摘要

痴呆症的日益流行使我们更好地了解其病理生理和治疗方式,以提高患者和护理人员的生活质量变得非常重要。阿尔茨海默病(AD)是一种神经退行性疾病,是老年人群中最常见的失忆性痴呆。AD的病理生理机制被广泛归因于淀粉样蛋白- β (Aβ)斑块的聚集和tau蛋白的过度磷酸化。初始治疗方式旨在以非特异性方式增加脑灌注。随后的治疗侧重于纠正大脑中的神经递质失衡。较新的药物通过作用于聚集的Aβ斑块来改变疾病的进展。然而,并非所有用于治疗AD的药物都获得了美国食品和药物管理局(FDA)的批准。本综述对fda批准的治疗阿尔茨海默病的药物进行了分类和总结,以便为研究人员和执业医生提供方便的参考。减轻痴呆症症状的药物可分为痴呆症行为和心理症状缓解剂(BPSD)和认知衰退缓解剂。BPSD缓解剂包括brexpiprazole(一种非典型抗精神病药物,每日一次,适合治疗痴呆患者的躁动)和suvorexant(一种用于治疗睡眠障碍的食欲素受体拮抗剂)。认知衰退缓解剂包括胆碱酯酶抑制剂,如多奈哌齐、利瓦司汀、加兰他明和谷氨酸抑制剂,如美金刚。多奈哌齐是最常用的处方药。它价格便宜,耐受性好,可以每天口服一次,也可以每周使用一次透皮贴片。它能提高乙酰胆碱水平,促进少突胶质细胞分化,还能防止β毒性。然而,由于心脏传导副作用的报道,需要定期进行心脏监测。利瓦斯汀需要每日两次口服剂量或每日一次更换透皮贴剂。它的心脏副作用比多奈哌齐少,但局部应用部位反应已被注意到。加兰他敏除了在短时间内改善认知症状外,还可以延缓bpsd的发展,并且由于具有多种代谢途径,药物相互作用最小。然而,心脏传导障碍必须密切监测。美金刚是一种谷氨酸调节剂,除了改善认知和神经保护外,还可以作为抗帕金森病药物和抗抑郁药,需要每天服用一次,以速释或缓释的形式口服片剂。治疗疾病的药物如aducanumab和lecanemab可以减轻Aβ负担。两者都通过与大脑中β斑块的纤维构象结合而起作用。这些药物有引起淀粉样蛋白相关成像异常的风险,特别是在携带ApoE4基因的人群中。Aducanumab每4周给药一次,lecanemab每2周给药一次。药物选择的决定必须在考虑药物的可获得性、患者的依从性(每日一次与每日多次剂量)、成本、特定合并症和特定患者的风险-收益比后做出。其他非药物治疗方式也必须采用,有一个整体的方法来治疗阿尔茨海默病。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Guidelines for pharmacotherapy in Alzheimer’s disease – A primer on FDA-approved drugs
The growing prevalence of dementia makes it important for us to better understand its pathophysiology and treatment modalities, to improve the quality of life of patients and caregivers. Alzheimer’s disease (AD), a neurodegenerative disease, is the most common form of amnestic dementia in the geriatric population. Pathophysiology of AD is widely attributed to aggregation of amyloid-beta (Aβ) plaques and hyperphosphorylation of tau proteins. Initial treatment modalities aimed to increase brain perfusion in a non-specific manner. Subsequent therapy focused on rectifying neurotransmitter imbalance in the brain. Newer drugs modify the progression of the disease by acting against aggregated Aβ plaques. However, not all drugs used in therapy of AD have been granted approval by the United States Food and Drug Administration (FDA). This review categorizes and summarizes the FDA-approved drugs in the treatment of AD in a manner that would make it a convenient reference for researchers and practicing physicians alike. Drugs that mitigate symptoms of dementia may be categorized into mitigators of Behavioral and Psychological Symptoms of Dementia (BPSD), and mitigators of cognitive decline. BPSD mitigators include brexpiprazole, an atypical antipsychotic with a once-daily dosage suited to treat agitation in dementia patients, and suvorexant, an orexin receptor antagonist used to treat sleep disturbances. Cognitive decline mitigators include cholinesterase inhibitors such as donepezil, rivastigmine, and galantamine and glutamate inhibitors such as memantine. Donepezil is the most commonly prescribed drug. It is cheap, well-tolerated, and may be prescribed orally once daily, or as a transdermal patch once weekly. It increases ACh levels, enhances oligodendrocyte differentiation and also protects against Aβ toxicity. However, regular cardiac monitoring is required due to reports of cardiac conduction side effects. Rivastigmine requires a twice-daily oral dosage or once-daily replacement of transdermal patch. It has fewer cardiac side effects than donepezil, but local application-site reactions have been noted. Galantamine, in addition to improving cognitive symptoms in a short span of time, also delays the development of BPSDs and has minimal drug-drug interactions by virtue of having multiple metabolic pathways. However, cardiac conduction disturbances must be closely monitored for. Memantine, a glutamate regulator, acts as an anti-Parkinsonian agent and an antidepressant, in addition to improving cognition and neuroprotection, and requires a once-daily dosage in the form of immediate-release or sustained-release oral tablets. Disease-modifying drugs such as aducanumab and lecanemab reduce the Aβ burden. Both act by binding with fibrillary conformations of Aβ plaques in the brain. These drugs have a risk of causing amyloid-related imaging abnormalities, especially in persons with ApoE4 gene. Aducanumab is administered once every 4 weeks and lecanemab once every 2 weeks. The decision on the choice of the drug must be made after considering the availability of drug, compliance of patient (once-daily vs. multiple doses daily), cost, specific comorbidities, and the risk-benefit ratio for the particular patient. Other non-pharmacological treatment modalities must also be adopted to have a holistic approach toward the treatment of AD.
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来源期刊
CiteScore
2.10
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