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额颞叶痴呆:最新证据及临床意义

Frontotemporal dementia: latest evidence and clinical implications.

作者信息

Young Juan Joseph, Lavakumar Mallika, Tampi Deena, Balachandran Silpa, Tampi Rajesh R

机构信息

Department of Psychiatry, MetroHealth Medical Center, Cleveland, OH, USA Case Western Reserve University, Cleveland, OH, USA.

Mercy Regional Medical Center, 3700 Kolbe Rd, Lorain, OH 44053, USA.

出版信息

Ther Adv Psychopharmacol. 2018 Jan;8(1):33-48. doi: 10.1177/2045125317739818. Epub 2017 Nov 10.

Abstract

BACKGROUND

Frontotemporal dementia (FTD) describes a cluster of neurocognitive syndromes that present with impairment of executive functioning, changes in behavior, and a decrease in language proficiency. FTD is the second most common form of dementia in those younger than 65 years and is expected to increase in prevalence as the population ages. This goal in our review is to describe advances in the understanding of neurobiological pathology, classification, assessment, and treatment of FTD syndromes.

METHODS

PubMed was searched to obtain reviews and studies that pertain to advancements in genetics, neurobiology, neuroimaging, classification, and treatment of FTD syndromes. Articles were chosen with a predilection to more recent preclinical/clinical trials and systematic reviews.

RESULTS

Recent reviews and trials indicate a significant advancement in the understanding of molecular and neurobiological clinical correlates to variants of FTD. Genetic and histopathologic markers have only recently been discovered in the past decade. Current therapeutic modalities are limited, with most studies reporting improvement in symptoms with nonpharmacological interventions. However, a small number of studies have reported improvement of behavioral symptoms with selective serotonin reuptake inhibitor (SSRI) treatment. Stimulants may help with disinhibition, apathy, and risk-taking behavior. Memantine and cholinesterase inhibitors have not demonstrated efficacy in ameliorating FTD symptoms. Antipsychotics have been used to treat agitation and psychosis, but safety concerns and side effect profiles limit utilization in the general FTD population. Nevertheless, recent breakthroughs in the understanding of FTD pathology have led to developments in pharmacological interventions that focus on producing treatments with autoimmune, genetic, and molecular targets.

CONCLUSION

FTD is an underdiagnosed group of neurological syndromes comprising multiple variants with distinct neurobiological profiles and presentations. Recent advances suggest there is an array of potential novel therapeutic targets, although data concerning their effectiveness are still preliminary or preclinical. Further studies are required to develop pharmacological interventions, as there are currently no US Food and Drug administration approved treatments to manage FTD syndromes.

摘要

背景

额颞叶痴呆(FTD)是一组神经认知综合征,表现为执行功能受损、行为改变和语言能力下降。FTD是65岁以下人群中第二常见的痴呆形式,预计随着人口老龄化其患病率会增加。我们综述的目的是描述在FTD综合征的神经生物学病理学、分类、评估和治疗方面的认识进展。

方法

检索PubMed以获取与FTD综合征的遗传学、神经生物学、神经影像学、分类和治疗进展相关的综述和研究。文章选择倾向于近期的临床前/临床试验和系统评价。

结果

近期的综述和试验表明,在理解FTD变体的分子和神经生物学临床相关性方面有了显著进展。遗传和组织病理学标志物在过去十年才刚刚被发现。目前的治疗方式有限,大多数研究报告非药物干预可改善症状。然而,少数研究报告选择性5-羟色胺再摄取抑制剂(SSRI)治疗可改善行为症状。兴奋剂可能有助于改善脱抑制、冷漠和冒险行为。美金刚和胆碱酯酶抑制剂尚未证明能改善FTD症状。抗精神病药物已被用于治疗激越和精神病,但安全性问题和副作用限制了其在一般FTD人群中的应用。尽管如此,最近在FTD病理学认识上的突破已导致针对自身免疫、遗传和分子靶点的药物干预的发展。

结论

FTD是一组诊断不足的神经综合征,包括多种具有不同神经生物学特征和表现的变体。近期进展表明有一系列潜在的新型治疗靶点,尽管关于其有效性的数据仍处于初步或临床前阶段。由于目前尚无美国食品药品监督管理局批准的治疗FTD综合征的药物,因此需要进一步研究以开发药物干预措施。

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