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Gut dysbiosis in Huntington’s disease: associations among gut microbiota cognitive performance and clinical outcomes

机译:亨廷顿疾病中的肠道脱泻:肠道微生物群认知性能和临床结果之间的关联

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摘要

Huntington’s disease is characterized by a triad of motor, cognitive and psychiatric impairments, as well as unintended weight loss. Although much of the research has focused on cognitive, motor and psychiatric symptoms, the extent of peripheral pathology and the relationship between these factors, and the core symptoms of Huntington’s disease, are relatively unknown. Gut microbiota are key modulators of communication between the brain and gut, and alterations in microbiota composition (dysbiosis) can negatively affect cognition, behaviour and affective function, and may be implicated in disease progression. Furthermore, gut dysbiosis was recently reported in Huntington’s disease transgenic mice. Our main objective was to characterize the gut microbiome in people with Huntington’s disease and determine whether the composition of gut microbiota are significantly related to clinical indicators of disease progression. We compared 42 Huntington’s disease gene expansion carriers, including 19 people who were diagnosed with Huntington’s disease (Total Functional Capacity > 6) and 23 in the premanifest stage, with 36 age- and gender-matched healthy controls. Participants were characterized clinically using a battery of cognitive tests and using results from 16S V3 to V4 rRNA sequencing of faecal samples to characterize the gut microbiome. For gut microbiome measures, we found significant differences in the microbial communities (beta diversity) based on unweighted UniFrac distance (P = 0.001), as well as significantly lower alpha diversity (species richness and evenness) between our combined Huntington’s disease gene expansion carrier group and healthy controls (P = 0.001). We also found major shifts in the microbial community structure at Phylum and Family levels, and identified functional pathways and enzymes affected in our Huntington’s disease gene expansion carrier group. Within the Huntington’s disease gene expansion carrier group, we also discovered associations among gut bacteria, cognitive performance and clinical outcomes. Overall, our findings suggest an altered gut microbiome in Huntington’s disease gene expansion carriers. These results highlight the importance of gut biomarkers and raise interesting questions regarding the role of the gut in Huntington’s disease, and whether it may be a potential target for future therapeutic intervention.
机译:亨廷顿的疾病的特点是三合会的电机,认知和精神障碍,以及意外减肥。虽然这项研究的大部分都集中在认知,运动和精神症状,外周病理的程度和这些因素之间的关系以及亨廷顿疾病的核心症状,相对不为人知。 Gut Microbiota是大脑和肠道之间的关键通信的关键调节剂,并且微生物群组成(疑难解失证)的改变可以对认知,行为和情感功能产生负面影响,并且可能涉及疾病进展。此外,最近在亨廷顿的疾病转基因小鼠中报道了肠道脱泻。我们的主要目标是在亨廷顿疾病中表征肠道微生物组,并确定肠道微生物的组成是否与疾病进展的临床指标有显着相关。我们将42株亨廷顿的疾病基因膨胀载体进行了比较,其中包括19名患有亨廷顿的疾病(总功能能力> 6)和23中的疫苗阶段,具有36次和性别匹配的健康对照。参与者在临床上使用一种认知测试进行临床表征,并使用16S V3至V4 rRNA测序的结果对粪便微生物组进行表征。对于肠道微生物梭测定的措施,我们发现基于未加权的Unifrac距离(P = 0.001)的微生物社区(β多样性)的显着差异,以及我们联合亨廷顿的疾病疾病基因扩增载体组之间的α多样性(物种丰富性和均匀性)显着降低和健康的对照(p = 0.001)。我们还发现了在文学和家庭水平的微生物群落结构中的主要变化,并确定了在亨廷顿疾病基因膨胀载体组中受影响的功能途径和酶。在亨廷顿的疾病基因膨胀载体组中,我们还发现了肠道细菌,认知性能和临床结果之间的关联。总体而言,我们的研究结果表明了亨廷顿疾病基因膨胀载体的改变的肠道微生物组。这些结果突出了肠道生物标志物的重要性,并提高了关于肠肠的作用的有趣问题,以及是否可能是未来治疗干预的潜在目标。

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