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Cochrane Database Syst Rev. 2019 Mar 13;3(3):CD012278. doi: 10.1002/14651858.CD012278.pub2.
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Computerised cognitive training for maintaining cognitive function in cognitively healthy people in late life.计算机化认知训练对维持老年人认知健康人群的认知功能的作用
Cochrane Database Syst Rev. 2019 Mar 13;3(3):CD012277. doi: 10.1002/14651858.CD012277.pub2.
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Vitamin and mineral supplementation for maintaining cognitive function in cognitively healthy people in mid and late life.维生素和矿物质补充剂对维持中老年认知健康人群的认知功能作用
Cochrane Database Syst Rev. 2018 Dec 17;12(12):CD011906. doi: 10.1002/14651858.CD011906.pub2.
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Vitamin and mineral supplementation for preventing dementia or delaying cognitive decline in people with mild cognitive impairment.维生素和矿物质补充剂用于预防痴呆或延缓轻度认知障碍患者的认知衰退。
Cochrane Database Syst Rev. 2018 Nov 1;11(11):CD011905. doi: 10.1002/14651858.CD011905.pub2.
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SYNERGIC TRIAL (SYNchronizing Exercises, Remedies in Gait and Cognition) a multi-Centre randomized controlled double blind trial to improve gait and cognition in mild cognitive impairment.协同试验(SYNchronizing Exercises、步态和认知疗法)——一项多中心随机对照双盲试验,旨在改善轻度认知障碍患者的步态和认知能力。
BMC Geriatr. 2018 Apr 16;18(1):93. doi: 10.1186/s12877-018-0782-7.
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Practice guideline update summary: Mild cognitive impairment: Report of the Guideline Development, Dissemination, and Implementation Subcommittee of the American Academy of Neurology.实践指南更新概要:轻度认知障碍:美国神经病学学会指南制定、传播和实施小组委员会的报告。
Neurology. 2018 Jan 16;90(3):126-135. doi: 10.1212/WNL.0000000000004826. Epub 2017 Dec 27.
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The Timecourse of Global Cognitive Gains from Supervised Computer-Assisted Cognitive Training: A Randomised, Active-Controlled Trial in Elderly with Multiple Dementia Risk Factors.监督式计算机辅助认知训练带来的整体认知提升的时间进程:一项针对有多种痴呆风险因素的老年人的随机、主动对照试验。
J Prev Alzheimers Dis. 2014;1(1):33-39. doi: 10.14283/jpad.2014.18.
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计算机化认知训练对预防轻度认知障碍患者痴呆症的作用

Computerised cognitive training for preventing dementia in people with mild cognitive impairment.

作者信息

Gates Nicola J, Vernooij Robin Wm, Di Nisio Marcello, Karim Salman, March Evrim, Martínez Gabriel, Rutjes Anne Ws

机构信息

Centre for Healthy Brain Ageing (CHeBA), University of New South Wales, Suite 407 185 Elizabeth Street, Sydney, NSW, Australia, 2000.

出版信息

Cochrane Database Syst Rev. 2019 Mar 13;3(3):CD012279. doi: 10.1002/14651858.CD012279.pub2.

DOI:10.1002/14651858.CD012279.pub2
PMID:30864747
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6415132/
Abstract

BACKGROUND

The number of people living with dementia is increasing rapidly. Clinical dementia does not develop suddenly, but rather is preceded by a period of cognitive decline beyond normal age-related change. People at this intermediate stage between normal cognitive function and clinical dementia are often described as having mild cognitive impairment (MCI). Considerable research and clinical efforts have been directed toward finding disease-modifying interventions that may prevent or delay progression from MCI to clinical dementia.

OBJECTIVES

To evaluate the effects of at least 12 weeks of computerised cognitive training (CCT) on maintaining or improving cognitive function and preventing dementia in people with mild cognitive impairment.

SEARCH METHODS

We searched to 31 May 2018 in ALOIS (www.medicine.ox.ac.uk/alois) and ran additional searches in MEDLINE, Embase, PsycINFO, CINAHL, ClinicalTrials.gov, and the WHO portal/ICTRP (www.apps.who.int/trialsearch) to identify published, unpublished, and ongoing trials.

SELECTION CRITERIA

We included randomised controlled trials (RCTs) and quasi-RCTs in which cognitive training via interactive computerised technology was compared with an active or inactive control intervention. Experimental computerised cognitive training (CCT) interventions had to adhere to the following criteria: minimum intervention duration of 12 weeks; any form of interactive computerised cognitive training, including computer exercises, computer games, mobile devices, gaming console, and virtual reality. Participants were adults with a diagnosis of mild cognitive impairment (MCI) or mild neurocognitive disorder (MND), or otherwise at high risk of cognitive decline.

DATA COLLECTION AND ANALYSIS

Two review authors independently extracted data and assessed risk of bias of the included RCTs. We expressed treatment effects as mean differences (MDs) or standardised mean differences (SMDs) for continuous outcomes and as risk ratios (RRs) for dichotomous outcomes. We used the GRADE approach to describe the overall quality of evidence for each outcome.

MAIN RESULTS

Eight RCTs with a total of 660 participants met review inclusion criteria. Duration of the included trials varied from 12 weeks to 18 months. Only one trial used an inactive control. Most studies were at unclear or high risk of bias in several domains. Overall, our ability to draw conclusions was hampered by very low-quality evidence. Almost all results were very imprecise; there were also problems related to risk of bias, inconsistency between trials, and indirectness of the evidence.No trial provided data on incident dementia. For comparisons of CCT with both active and inactive controls, the quality of evidence on our other primary outcome of global cognitive function immediately after the intervention period was very low. Therefore, we were unable to draw any conclusions about this outcome.Due to very low quality of evidence, we were also unable to determine whether there was any effect of CCT compared to active control on our secondary outcomes of episodic memory, working memory, executive function, depression, functional performance, and mortality. We found low-quality evidence suggesting that there is probably no effect on speed of processing (SMD 0.20, 95% confidence interval (CI) -0.16 to 0.56; 2 studies; 119 participants), verbal fluency (SMD -0.16, 95% CI -0.76 to 0.44; 3 studies; 150 participants), or quality of life (mean difference (MD) 0.40, 95% CI -1.85 to 2.65; 1 study; 19 participants).When CCT was compared with inactive control, we obtained data on five secondary outcomes, including episodic memory, executive function, verbal fluency, depression, and functional performance. We found very low-quality evidence; therefore, we were unable to draw any conclusions about these outcomes.

AUTHORS' CONCLUSIONS: Currently available evidence does not allow us to determine whether or not computerised cognitive training will prevent clinical dementia or improve or maintain cognitive function in those who already have evidence of cognitive impairment. Small numbers of trials, small samples, risk of bias, inconsistency between trials, and highly imprecise results mean that it is not possible to derive any implications for clinical practice, despite some observed large effect sizes from individual studies. Direct adverse events are unlikely to occur, although the time and sometimes the money involved in computerised cognitive training programmes may represent significant burdens. Further research is necessary and should concentrate on improving methodological rigour, selecting suitable outcomes measures, and assessing generalisability and persistence of any effects. Trials with long-term follow-up are needed to determine the potential of this intervention to reduce the risk of dementia.

摘要

背景

痴呆症患者数量正在迅速增加。临床痴呆并非突然发生,而是在一段超出正常年龄相关变化的认知衰退期之后出现。处于正常认知功能与临床痴呆之间这一中间阶段的人通常被描述为患有轻度认知障碍(MCI)。大量研究和临床工作致力于寻找可能预防或延缓从MCI进展至临床痴呆的疾病修饰干预措施。

目的

评估至少12周的计算机化认知训练(CCT)对维持或改善轻度认知障碍患者认知功能及预防痴呆的效果。

检索方法

我们检索至2018年5月31日的ALOIS(www.medicine.ox.ac.uk/alois),并在MEDLINE、Embase、PsycINFO、CINAHL、ClinicalTrials.gov和WHO门户网站/ICTRP(www.apps.who.int/trialsearch)进行了额外检索以识别已发表、未发表及正在进行的试验。

入选标准

我们纳入了随机对照试验(RCT)和半随机对照试验,其中通过交互式计算机技术进行的认知训练与积极或非积极对照干预进行比较。实验性计算机化认知训练(CCT)干预必须符合以下标准:最短干预持续时间为12周;任何形式的交互式计算机化认知训练,包括计算机练习、电脑游戏、移动设备、游戏机和虚拟现实。参与者为诊断为轻度认知障碍(MCI)或轻度神经认知障碍(MND)的成年人,或其他有认知衰退高风险的人。

数据收集与分析

两位综述作者独立提取数据并评估纳入的RCT的偏倚风险。我们将治疗效果表示为连续结局的平均差(MDs)或标准化平均差(SMDs),以及二分结局的风险比(RRs)。我们使用GRADE方法描述每个结局的总体证据质量。

主要结果

八项RCT共660名参与者符合综述纳入标准。纳入试验的持续时间从12周至18个月不等。只有一项试验使用了非积极对照。大多数研究在几个领域存在不明确或高偏倚风险。总体而言,极低质量的证据阻碍了我们得出结论。几乎所有结果都非常不精确;还存在与偏倚风险、试验间不一致性以及证据间接性相关的问题。没有试验提供关于新发痴呆的数据。对于CCT与积极和非积极对照的比较,干预期后我们另一个主要结局全球认知功能的证据质量非常低。因此,我们无法就此结局得出任何结论。由于证据质量极低,我们也无法确定与积极对照相比,CCT对我们的次要结局情景记忆、工作记忆、执行功能、抑郁、功能表现和死亡率是否有任何影响。我们发现低质量证据表明可能对处理速度(SMD 0.20,95%置信区间(CI)-0.16至0.56;2项研究;119名参与者)、言语流畅性(SMD -0.16,95%CI -0.76至0.44;3项研究;150名参与者)或生活质量(平均差(MD)0.40,95%CI -1.85至2.65;1项研究;19名参与者)没有影响。当将CCT与非积极对照进行比较时,我们获得了关于五个次要结局的数据,包括情景记忆、执行功能、言语流畅性、抑郁和功能表现。我们发现证据质量极低;因此,我们无法就这些结局得出任何结论。

作者结论

目前可得的证据无法让我们确定计算机化认知训练是否能预防临床痴呆,或改善或维持已有认知障碍证据者的认知功能。试验数量少、样本量小、偏倚风险、试验间不一致性以及高度不精确的结果意味着尽管个别研究观察到一些较大的效应量,但仍无法得出对临床实践的任何启示。直接不良事件不太可能发生,尽管计算机化认知训练项目所涉及的时间以及有时的费用可能构成重大负担。有必要进行进一步研究,应专注于提高方法学严谨性、选择合适的结局测量指标以及评估任何效应的普遍性和持续性。需要进行长期随访试验以确定这种干预降低痴呆风险的潜力。