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同型半胱氨酸降低 B 族维生素治疗轻度认知障碍的认知和临床结局:一项随机对照试验。

Cognitive and clinical outcomes of homocysteine-lowering B-vitamin treatment in mild cognitive impairment: a randomized controlled trial.

机构信息

OPTIMA, Nuffield Department of Clinical Medicine, University of Oxford, Oxford, UK.

出版信息

Int J Geriatr Psychiatry. 2012 Jun;27(6):592-600. doi: 10.1002/gps.2758. Epub 2011 Jul 21.

Abstract

BACKGROUND

Homocysteine is a risk factor for Alzheimer's disease. In the first report on the VITACOG trial, we showed that homocysteine-lowering treatment with B vitamins slows the rate of brain atrophy in mild cognitive impairment (MCI). Here we report the effect of B vitamins on cognitive and clinical decline (secondary outcomes) in the same study.

METHODS

This was a double-blind, single-centre study, which included participants with MCI, aged ≥ 70 y, randomly assigned to receive a daily dose of 0.8 mg folic acid, 0.5 mg vitamin B(12) and 20 mg vitamin B(6) (133 participants) or placebo (133 participants) for 2 y. Changes in cognitive or clinical function were analysed by generalized linear models or mixed-effects models.

RESULTS

The mean plasma total homocysteine was 30% lower in those treated with B vitamins relative to placebo. B vitamins stabilized executive function (CLOX) relative to placebo (P = 0.015). There was significant benefit of B-vitamin treatment among participants with baseline homocysteine above the median (11.3 µmol/L) in global cognition (Mini Mental State Examination, P < 0.001), episodic memory (Hopkins Verbal Learning Test-delayed recall, P = 0.001) and semantic memory (category fluency, P = 0.037). Clinical benefit occurred in the B-vitamin group for those in the upper quartile of homocysteine at baseline in global clinical dementia rating score (P = 0.02) and IQCODE score (P = 0.01).

CONCLUSION

In this small intervention trial, B vitamins appear to slow cognitive and clinical decline in people with MCI, in particular in those with elevated homocysteine. Further trials are needed to see if this treatment will slow or prevent conversion from MCI to dementia.

摘要

背景

同型半胱氨酸是阿尔茨海默病的一个风险因素。在 VITACOG 试验的首次报告中,我们表明,用 B 族维生素降低同型半胱氨酸的治疗可以减缓轻度认知障碍(MCI)患者的脑萎缩速度。在这里,我们报告同一项研究中 B 族维生素对认知和临床衰退(次要结果)的影响。

方法

这是一项双盲、单中心研究,纳入了年龄≥70 岁的 MCI 患者,随机分配接受每日剂量为 0.8mg 叶酸、0.5mg 维生素 B(12) 和 20mg 维生素 B(6)(133 名参与者)或安慰剂(133 名参与者)治疗 2 年。通过广义线性模型或混合效应模型分析认知或临床功能的变化。

结果

与安慰剂相比,B 族维生素治疗组的血浆总同型半胱氨酸降低了 30%。B 族维生素相对于安慰剂稳定了执行功能(CLOX)(P = 0.015)。在基线同型半胱氨酸高于中位数(11.3µmol/L)的参与者中,B 族维生素治疗有显著获益,表现在总体认知(简易精神状态检查,P<0.001)、情景记忆(霍普金斯词语学习测验-延迟回忆,P=0.001)和语义记忆(类别流畅性,P=0.037)方面。在基线时同型半胱氨酸处于上四分位数的参与者中,B 族维生素治疗组在总体临床痴呆评定量表评分(P=0.02)和 IQCODE 评分(P=0.01)方面出现了临床获益。

结论

在这项小型干预试验中,B 族维生素似乎可以减缓 MCI 患者的认知和临床衰退,特别是那些同型半胱氨酸升高的患者。需要进一步的试验来确定这种治疗是否会减缓或预防 MCI 向痴呆的转化。

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