a Neurodegenerative Disease Unit, Department of Basic Medical Sciences, Neuroscience and Sense Organs , University of Bari "Aldo Moro" , Bari , Italy.
b Department of Clinical Research in Neurology, Center for Neurodegenerative Diseases and the Aging Brain , University of Bari "Aldo Moro", "Pia Fondazione Cardinale G. Panico" , Lecce , Italy.
Expert Opin Pharmacother. 2019 Jun;20(9):1091-1107. doi: 10.1080/14656566.2019.1598377. Epub 2019 Apr 19.
Frontotemporal dementia (FTD) is a heterogeneous clinical entity that includes several disorders characterized by different cellular mechanisms. Distinctive clinical features in FTD include behavioral, affective, and cognitive symptoms. Unfortunately, little progress has been made over the past 20 years in terms of the development of effective disease-modifying drugs with the currently available symptomatic treatments having limited clinical utility.
This article reviews the principal pharmacological intervention studies for FTD. These are predominantly randomized clinical trials and include symptomatic treatments and potential disease-modifying drugs.
There is insufficient evidence on effective treatments for FTD and studies with better methodological backgrounds are needed. Most studies reporting therapeutic benefits were conducted with selective serotonin reuptake inhibitors, while anti-dementia drugs have been ineffective in FTD. Since the underlying pathology of FTD mostly consists of abnormal tau protein or TDP-43 aggregates, treatments are being developed to interfere with their aggregation process or with the clearance of these proteins. Furthermore, disease-modifying treatments remain years away as demonstrated by the recent negative Phase III findings of a tau aggregation inhibitor (LMTM) for treating the behavioral variant of FTD. The results from current ongoing Phase I/II trials will hopefully give light to future treatment options.
额颞叶痴呆(FTD)是一种异质性的临床实体,包括几种以不同细胞机制为特征的疾病。FTD 的独特临床特征包括行为、情感和认知症状。不幸的是,在过去的 20 年中,在开发有效的疾病修饰药物方面几乎没有取得进展,而目前可用的对症治疗方法的临床实用性有限。
本文回顾了 FTD 的主要药物干预研究。这些主要是随机临床试验,包括对症治疗和潜在的疾病修饰药物。
目前针对 FTD 的有效治疗方法的证据不足,需要进行具有更好方法学背景的研究。大多数报告治疗益处的研究都是使用选择性 5-羟色胺再摄取抑制剂进行的,而抗痴呆药物在 FTD 中无效。由于 FTD 的潜在病理主要由异常的 tau 蛋白或 TDP-43 聚集体组成,因此正在开发治疗方法来干扰其聚集过程或清除这些蛋白质。此外,正如最近针对治疗 FTD 行为变异型的 tau 聚集抑制剂(LMTM)的 III 期阴性研究结果所示,疾病修饰治疗仍遥遥无期。目前正在进行的 I/II 期试验的结果有望为未来的治疗选择提供启示。
