首页> 外文期刊>American Journal of Physiology >Hormones, Neurotransmitters, Growth Factors, Receptors, and Signaling: Involvement of gut microbiota in association between GLP-l/GLP-1 receptor expression and gastrointestinal motility
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Hormones, Neurotransmitters, Growth Factors, Receptors, and Signaling: Involvement of gut microbiota in association between GLP-l/GLP-1 receptor expression and gastrointestinal motility

机译:激素,神经递质,生长因子,受体和信号传导:Gut Microbiota参与GLP-L / GLP-1受体表达和胃肠运动性之间的关联

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Yang M, Fukui H, Eda H, Xu X, Kitayama Y, Hara K, Kodani M, Tomita T, Oshima T, Watari J, Miwa H. Involvement of gut microbiota in association between GLP-1/GLP-1 receptor expression and gastrointestinal motility. Am J Physiol Gastrointest Liver Physiol 312: G367-G373, 2017. First published February 2, 2017; doi: l0.1152/ajpgi.00232.2016.—The microbiota in the gut is known to play a pivotal role in host physiology by interacting with the immune and neuroendocrine systems in gastrointestinal (GI) tissues. Gluca-gon-like peptide 1 (GLP-1), a gut hormone, is involved in metabolism as well as GI motility. We examined how gut microbiota affects the link between GLP-l/GLP-1 receptor (GLP-1R) expression and motility of the GI tract. Germ-free (GF) mice (6 wk old) were orally administered a fecal bacterial suspension prepared from specific pathogen-free (SPF) mice, and then after fecal transplantation (FT) GI tissues were obtained from the GF mice at various time points. The expression of GLP-1 and its receptor was examined by immunohis-tochemistry, and gastrointestinal transit time (GITT) was measured by administration of carmine red solution. GLP-1 was expressed in endocrine cells in the colonic mucosa, and GLP-1R was expressed in myenteric neural cells throughout the GI wall. GLP-1R-positive cells throughout the GI wall were significantly fewer in GF mice with FT than in GF mice without gut microbiota reconstitution. GITT was significantly shorter in GF mice with FT than in control GF mice without FT and correlated with the number of GLP-1 R-positive cells throughout the GI wall. GITT was significantly longer in GF control mice than in SPF mice. When those mice were treated with GLP-1 agonist extending GITT was significantly longer in the GF mice. The gut microbiota may accelerate or at least modify GI motility while suppressing GLP-1R expression in myenteric neural cells throughout the GI tract. NEW & NOTEWORTHY The gut microbiota has been intensively studied, because it plays a pivotal role in various aspects of host physiology. On the other hand, glucagon-like peptide 1 (GLP-1) plays important roles in metabolism as well as gastrointestinal motility. In the present study, we have suggested that the gut microbiota accelerates gastrointestinal motility while suppressing the expression of GLP-1 receptor in myenteric neural cells throughout the gastrointestinal tract. We believe that this article is very timely and suggestive work.
机译:Yang M,Fukui H,Eda H,Xu X,Kitayama Y,Hara K,Kodani M,Tomita T,Oshima T,Watari J,MiWa H. Gut Microbiota在GLP-1 / GLP-1受体表达之间的关系中的参与胃肠道运动。 AM j Physiol Gastropeptest Liver Physiol 312:G367-G373,20177。2017年2月2日第一次出版; DOI:L0.1152 / AJPGI.00232.2016 - 肠道中的微生物群是通过与胃肠道(GI)组织中的免疫和神经分区系统相互作用来发挥宿主生理中的枢转作用。葡萄糖般的肽1(GLP-1),肠道激素,参与代谢和GI运动。我们检查了Gut Microbiota如何影响GLP-L / GLP-1受体(GLP-1R)表达和GI道的动力之间的联系。口服无菌(GF)小鼠(6WK旧)口服由无菌无菌(SPF)小鼠制备的粪便细菌悬浮液,然后在各个时间点从GF小鼠获得粪便移植(FT)GI组织之后。通过免疫阳离子 - 转化检测GLP-1及其受体的表达,通过施用胭脂红溶液测量胃肠传递时间(GITT)。 GLP-1在结肠粘膜中的内分泌细胞中表达,GLP-1R在整个GI壁的神经元神经细胞中表达。 Gi壁的GLP-1R阳性细胞在GF小鼠中显着较小,FT小鼠比没有肠道微生物重构的GF小鼠。 GF小鼠GF小鼠的GF小鼠显着短,而不是在没有FT的对照GF小鼠中并且与整个Gi壁的GLP-1 R阳性细胞数相关。 GF对小鼠的GF在SPF小鼠中明显更长。当用GLP-1处理那些小鼠的小鼠时,延伸GF在GF小鼠中显着更长。肠道微生物A可以加速或至少改变GI运动,同时抑制整个GI的神经细胞中的GLP-1R表达。新的和值得注意的肠道微生物群已经深入研究,因为它在宿主生理学的各个方面发挥着关键作用。另一方面,胰高血糖素样肽1(GLP-1)在新陈代谢和胃肠运动中起重要作用。在本研究中,我们建议肠道微生物群加速胃肠运动,同时抑制在整个胃肠道整个胃肠道中的神经元神经细胞中GLP-1受体的表达。我们认为这篇文章是非常及时的,暗示的工作。

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