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阿尔茨海默病潜在脑微生物组研究:研究偏倚的影响。

Investigation of Potential Brain Microbiome in Alzheimer's Disease: Implications of Study Bias.

机构信息

Department of Neurology, Icahn School of Medicine at Mount Sinai, New York, NY, USA.

Diversigen, Inc., Houston, TX, USA.

出版信息

J Alzheimers Dis. 2020;75(2):559-570. doi: 10.3233/JAD-191328.

Abstract

BACKGROUND

Dysbiotic microbiota in the gastrointestinal tract promotes and aggravates neurodegenerative disorders. Alzheimer's disease (AD) has been shown to correlate to dysbiotic bacteria and the immune, metabolic, and endocrine abnormalities associated with abnormal gut-brain-axis signaling. Recent reports also indicate that brain dysbacteriosis may play a role in AD pathogenesis.

OBJECTIVE

To evaluate the presence and differences of brain-region dependent microbiomes in control and AD subjects and the contribution of study bias.

METHODS

Two independent cohorts of postmortem AD brain samples were collected from separate locations, processed with different extraction protocols and investigated for the presence of bacterial DNA indicative of a brain microbiome with V4 16S next generation sequencing.

RESULTS

In both cohorts, few differences between the control and AD groups were observed in terms of alpha and beta diversities, phyla and genera proportions. Independent of study in both AD and control subjects the most abundant phyla were Proteobacteria, Firmicutes, Actinobacteria, and Bacteroidetes. Variations in beta diversity between hippocampal and cerebellum samples were observed indicating an impact of brain region on the presence of microbial DNA. Importantly, differences in alpha and beta diversities between the two independent cohorts were found indicating a significant cohort- and processing-dependent effect on the microbiome. Finally, there were cohort-specific correlations between the gut microbiome and subject demographics indicate that postmortem interval may have a significant impact on brain microbiome determination.

CONCLUSIONS

Regardless of the study bias, this study concludes that bacterial DNA can be isolated from the human brain suggesting that a brain microbiome may exist; however, more studies are required to understand the variation in AD.

摘要

背景

胃肠道中的失调微生物群会促进和加重神经退行性疾病。阿尔茨海默病(AD)与失调细菌以及与异常肠道-大脑轴信号相关的免疫、代谢和内分泌异常相关。最近的报告还表明,大脑细菌失调可能在 AD 发病机制中起作用。

目的

评估对照和 AD 受试者中存在且不同的大脑依赖微生物组,以及研究偏倚的贡献。

方法

从不同的位置收集了两个独立的 AD 大脑样本的队列,使用不同的提取方案进行处理,并使用 V4 16S 下一代测序来研究存在指示大脑微生物组的细菌 DNA。

结果

在两个队列中,对照和 AD 组之间在 alpha 和 beta 多样性、门和属比例方面观察到的差异很小。独立于研究,在 AD 和对照受试者中最丰富的门是变形菌门、厚壁菌门、放线菌门和拟杆菌门。在海马和小脑样本之间观察到 beta 多样性的变化,表明大脑区域对微生物 DNA 的存在有影响。重要的是,在两个独立队列之间发现了 alpha 和 beta 多样性的差异,表明微生物组存在显著的队列和处理依赖性影响。最后,肠道微生物组与受试者人口统计学之间存在队列特异性相关性,表明死后间隔时间可能对大脑微生物组的确定有重大影响。

结论

无论存在研究偏倚,本研究都得出结论,细菌 DNA 可以从人类大脑中分离出来,表明可能存在大脑微生物组;然而,需要更多的研究来了解 AD 的变化。

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