Department of Brain Sciences, Imperial College London, London, UK.
Department of Neurology, Amsterdam UMC, University of Amsterdam, Amsterdam, Netherlands.
Cochrane Database Syst Rev. 2022 Jul 14;7(7):CD012269. doi: 10.1002/14651858.CD012269.pub2.
Cerebral small vessel disease is a progressive disease of the brain's deep perforating blood vessels. It is usually diagnosed based on lesions seen on brain imaging. Cerebral small vessel disease is a common cause of stroke but can also cause a progressive cognitive decline. As antithrombotic therapy is an established treatment for stroke prevention, we sought to determine whether antithrombotic therapy might also be effective in preventing cognitive decline in people with small vessel disease.
To assess the effects of antithrombotic therapy for prevention of cognitive decline in people with small vessel disease on neuroimaging but without dementia.
We searched ALOIS, the Cochrane Dementia and Cognitive Improvement Review Group's Specialised Register, and the Cochrane Stroke Group's Specialised Register; the most recent search was on 21 July 2021. We also searched MEDLINE, Embase, four other databases and two trials registries. We searched the reference lists of the articles retrieved from these searches. As trials with a stroke focus may include relevant subgroup data, we complemented these searches with a focussed search of all antithrombotic titles in the Cochrane Stroke Group database. SELECTION CRITERIA: We included randomised controlled trials (RCT) of people with neuroimaging evidence of at least mild cerebral small vessel disease (defined here as white matter hyperintensities, lacunes of presumed vascular origin and subcortical infarcts) but with no evidence of dementia. The trials had to compare antithrombotic therapy of minimum 24 weeks' duration to no antithrombotic therapy (either placebo or treatment as usual), or compare different antithrombotic treatment regimens. Antithrombotic therapy could include antiplatelet agents (as monotherapy or combination therapy), anticoagulants or a combination.
Two review authors independently screened all the titles identified by the searches. We assessed full texts for eligibility for inclusion according to our prespecified selection criteria, extracted data to a proforma and assessed risk of bias using the Cochrane tool for RCTs. We evaluated the certainty of evidence using GRADE. Due to heterogeneity across included participants, interventions and outcomes of eligible trials, it was not possible to perform meta-analyses.
We included three RCTs (3384 participants). One study investigated the effect of antithrombotic therapy in participants not yet on antithrombotic therapy; two studies investigated the effect of additional antithrombotic therapy, one in a population already taking a single antithrombotic agent and one in a mixed population (participants on an antithrombotic drug and antithrombotic-naive participants). Intervention and follow-up durations varied from 24 weeks to four years. Jia 2016 was a placebo-controlled trial assessing 24 weeks of treatment with DL-3-n-butylphthalide (a compound with multimodal actions, including a putative antiplatelet effect) in 280 Chinese participants with vascular cognitive impairment caused by subcortical ischaemic small vessel disease, but without dementia. There was very low-certainty evidence for a small difference in cognitive test scores favouring treatment with DL-3-n-butylphthalide, as measured by the 12-item Alzheimer's Disease Assessment Scale-Cognitive subscale (adjusted mean difference -1.07, 95% confidence interval (CI) -2.02 to -0.12), but this difference may not be clinically relevant. There was also very low-certainty evidence for greater proportional improvement measured with the Clinician Interview-Based Impression of Change-Plus Caregiver Input (57% with DL-3-n-butylphthalide versus 42% with placebo; P = 0.01), but there was no difference in other measures of cognition (Mini-Mental State Examination and Clinical Dementia Rating) or function. There was no evidence of a difference in adverse events between treatment groups. The SILENCE RCT compared antithrombotic therapy (aspirin) and placebo during four years of treatment in 83 participants with 'silent brain infarcts' who were on no prior antithrombotic therapy. There was very low-certainty evidence for no difference between groups across various measures of cognition and function, rates of stroke or adverse events. The Secondary Prevention of Subcortical Stroke Study (SPS3) compared dual antiplatelet therapy (clopidogrel plus aspirin) to aspirin alone in 3020 participants with recent lacunar stroke. There was low-certainty evidence of no effect on cognitive outcomes as measured by the Cognitive Abilities Screening Instruments (CASI) assessed annually over five years. There was also low-certainty evidence of no difference in the annual incidence of mild cognitive decline between the two treatment groups (9.7% with dual antiplatelet therapy versus 9.9% with aspirin), or the annual stroke recurrence rate (2.5% with dual antiplatelet therapy versus 2.7% with aspirin). Bleeding risk may be higher with dual antiplatelet therapy (hazard ratio (HR) 2.15, 95% CI 1.49 to 3.11; low certainty evidence), but there may be no significant increase in intracerebral bleeding risk (HR 1.52, 95% CI 0.79 to 2.93; low-certainty evidence). None of the included trials assessed the incidence of new dementia.
AUTHORS' CONCLUSIONS: We found no convincing evidence to suggest any clinically relevant cognitive benefit of using antithrombotic therapy in addition to standard treatment in people with cerebral small vessel disease but without dementia, but there may be an increased bleeding risk with this approach. There was marked heterogeneity across the trials and the certainty of the evidence was generally poor.
脑小血管病是一种大脑深部穿通血管的进行性疾病。通常根据脑影像学所见的病变进行诊断。脑小血管病是中风的常见原因,但也可导致认知能力逐渐下降。由于抗血栓治疗是预防中风的既定治疗方法,我们试图确定抗血栓治疗是否也可能预防小血管疾病患者的认知能力下降。
评估抗血栓治疗对预防无痴呆小血管病患者认知能力下降的效果。
我们检索了 ALOIS、Cochrane 痴呆和认知改善综述组的专着登记册以及 Cochrane 卒中组的专着登记册;最近的一次检索是在 2021 年 7 月 21 日。我们还检索了 MEDLINE、Embase、其他四个数据库和两个试验注册处。我们还对检索到的文章的参考文献列表进行了检索。由于专注于卒中的试验可能包含相关亚组数据,因此我们补充了对 Cochrane 卒中组数据库中所有抗血栓药物标题的重点搜索。
我们纳入了有神经影像学证据显示至少有轻度脑小血管病(这里定义为脑白质高信号、血管源性腔隙和皮质下梗死)但无痴呆的随机对照试验(RCT)。试验必须比较至少 24 周的抗血栓治疗与无抗血栓治疗(安慰剂或常规治疗),或比较不同的抗血栓治疗方案。抗血栓治疗可以包括抗血小板药物(单药或联合治疗)、抗凝剂或联合治疗。
两名综述作者独立筛选了所有搜索结果的标题。我们根据预先确定的选择标准评估了所有全文的纳入资格,根据预定义的方案提取数据,并使用 Cochrane 工具评估了 RCT 的偏倚风险。我们使用 GRADE 评估证据的确定性。由于纳入试验的参与者、干预措施和结局存在异质性,因此无法进行荟萃分析。
我们纳入了三项 RCT(3384 名参与者)。一项研究调查了抗血栓治疗在尚未接受抗血栓治疗的参与者中的效果;两项研究调查了额外抗血栓治疗的效果,一项研究在已经服用单一抗血栓药物的人群中进行,另一项研究在混合人群(服用抗血栓药物和抗血栓药物未使用者)中进行。干预和随访时间从 24 周到 4 年不等。Jia 2016 是一项安慰剂对照试验,评估了 280 名中国参与者在皮质下缺血性小血管病引起的血管性认知障碍(但无痴呆)中接受为期 24 周的 DL-3-n-丁基苯酞(一种具有多种作用的化合物,包括潜在的抗血小板作用)治疗的效果。有非常低确定性证据表明,DL-3-n-丁基苯酞治疗组的认知测试评分略有改善,以阿尔茨海默病评估量表-认知子量表(调整后的平均差值-1.07,95%置信区间(CI)-2.02 至-0.12)衡量,但这种差异可能无临床意义。也有非常低确定性证据表明,使用临床医生访谈为基础的变化评估-加照顾者输入(57%接受 DL-3-n-丁基苯酞治疗,42%接受安慰剂治疗;P=0.01)的比例改善更大,但其他认知(简易精神状态检查和临床痴呆评定)或功能测量没有差异。治疗组之间的不良事件没有差异。SILENCE RCT 在 83 名接受无抗血栓治疗的“沉默性脑梗死”患者中比较了为期四年的抗血栓治疗(阿司匹林)和安慰剂治疗。在各种认知和功能、卒中发生率或不良事件方面,两组之间没有差异,证据确定性非常低。次级预防皮质下卒中研究(SPS3)比较了氯吡格雷联合阿司匹林与单独使用阿司匹林在 3020 名近期腔隙性卒中患者中的效果。使用认知能力筛查工具(CASI)每年评估一次,为期五年,认知结局没有效果,证据确定性低。在两组之间,每年轻度认知下降的发生率(双联抗血小板治疗组为 9.7%,阿司匹林组为 9.9%)或每年卒中复发率(双联抗血小板治疗组为 2.5%,阿司匹林组为 2.7%)也没有差异,证据确定性低。双联抗血小板治疗可能会增加出血风险(风险比(HR)2.15,95%CI 1.49 至 3.11;低确定性证据),但颅内出血风险可能没有显著增加(HR 1.52,95%CI 0.79 至 2.93;低确定性证据)。纳入的试验均未评估新发痴呆的发生率。
我们没有发现任何令人信服的证据表明,在有小血管病但无痴呆的患者中,除了标准治疗外,使用抗血栓治疗会带来任何有临床意义的认知获益,但这种方法可能会增加出血风险。试验之间存在明显的异质性,证据的确定性总体较差。
