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Short‐chain fatty acids: microbial metabolites that alleviate stress‐induced brain–gut axis alterations

机译:短链脂肪酸:微生物代谢物,减轻应力诱导的脑压轴改变

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Key points Chronic (psychosocial) stress changes gut microbiota composition, as well as inducing behavioural and physiological deficits. The microbial metabolites short‐chain fatty acids (SCFAs) have been implicated in gastrointestinal functional, (neuro)immune regulation and host metabolism, but their role in stress‐induced behavioural and physiological alterations is poorly understood. Administration of SCFAs to mice undergoing psychosocial stress alleviates enduring alterations in anhedonia and heightened stress‐responsiveness, as well as stress‐induced increases in intestinal permeability. In contrast, chronic stress‐induced alterations in body weight gain, faecal SCFAs and the gene expression of the SCFA receptors FFAR2 and FFAR3 remained unaffected by SCFA supplementation. These results present novel insights into mechanisms underpinning the influence of the gut microbiota on brain homeostasis, behaviour and host metabolism, informing the development of microbiota‐targeted therapies for stress‐related disorders. Abstract There is a growing recognition of the involvement of the gastrointestinal microbiota in the regulation of physiology and behaviour. Microbiota‐derived metabolites play a central role in the communication between microbes and their host, with short‐chain fatty acids (SCFAs) being perhaps the most studied. SCFAs are primarily derived from fermentation of dietary fibres and play a pivotal role in host gut, metabolic and immune function. All these factors have previously been demonstrated to be adversely affected by stress. Therefore, we sought to assess whether SCFA supplementation could counteract the enduring effects of chronic psychosocial stress. C57BL/6J male mice received oral supplementation of a mixture of the three principle SCFAs (acetate, propionate and butyrate). One week later, mice underwent 3?weeks of repeated psychosocial stress, followed by a comprehensive behavioural analysis. Finally, plasma corticosterone, faecal SCFAs and caecal microbiota composition were assessed. SCFA treatment alleviated psychosocial stress‐induced alterations in reward‐seeking behaviour, and increased responsiveness to an acute stressor and in vivo intestinal permeability. In addition, SCFAs exhibited behavioural test‐specific antidepressant and anxiolytic effects, which were not present when mice had also undergone psychosocial stress. Stress‐induced increases in body weight gain, faecal SCFAs and the colonic gene expression of the SCFA receptors free fatty acid receptors 2 and 3 remained unaffected by SCFA supplementation. Moreover, there were no collateral effects on caecal microbiota composition. Taken together, these data show that SCFA supplementation alleviates selective and enduring alterations induced by repeated psychosocial stress and these data may inform future research into microbiota‐targeted therapies for stress‐related disorders.
机译:关键点慢性(心理社会)应力改变肠道微生物群组成,以及诱导行为和生理缺陷。微生物代谢物短链脂肪酸(SCFA)涉及胃肠功能,(神经)免疫调节和宿主代谢,但它们在应激引起的行为和生理改变中的作用很差。对经历心理社会压力的小鼠的小鼠施用SCFA可减轻持续的厌氧和胁迫响应性的改变,以及肠道渗透性的应激诱导的增加。相反,慢性应激诱导的体重增加,粪便SCFA和SCFA受体FFAR2和FFAR3的基因表达的变化仍未受到SCFA补充的影响。这些结果将新颖的见解融入了肠道微生物症对脑稳态,行为和宿主代谢的影响的机制,了解对压力相关疾病的微生物群靶向疗法的发展。摘要越来越彰显胃肠微生物群在生理和行为调节中的累及。 Microbiota衍生的代谢物在微生物和宿主之间的沟通中起着核心作用,短链脂肪酸(SCFA)也许是最多的研究。 SCFA主要来自膳食纤维的发酵,并在宿主肠道,代谢和免疫功能中发挥枢轴作用。先前已经证明所有这些因素受到压力的不利影响。因此,我们试图评估SCFA补充是否可以抵消慢性心理社会压力的持久影响。 C57BL / 6J雄性小鼠接受了口服补充了三种原理SCFA(醋酸盐,丙酸盐和丁酸酯)的混合物。一周后,小鼠接受了3个?几周重复的心理社会压力,其次是全面的行为分析。最后,评估了血浆皮质酮,粪便SCFA和粘颈微生物群组合物。 SCFA治疗缓解了精神病的应激引起的奖励行为的改变,以及对急性压力源的反应性和体内肠道渗透性增加。此外,SCFA表现出行为特异性的抗抑郁药和抗焦虑作用,当小鼠也经历了心理社会应激时,这是不存在的。应激诱导的体重增加,粪便SCFA和SCFA受体的结肠基因表达的增加的脂肪酸受体2和3的含量不受SCFA补充的影响。此外,粘颈微生物群组合物没有抵押品效应。这些数据集中在一起,SCFA补充减轻了反复心理社会应激引起的选择性和持久的改变,这些数据可能会通知未来的对微生物群针对应力相关疾病的疗法。

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