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The circadian clock regulates the diurnal levels of microbial short-chain fatty acids and their rhythmic effects on colon contractility in mice

机译:昼夜节奏调节微生物短链脂肪酸的昼夜水平及其对小鼠结肠收缩性的节奏作用

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Aim The microbiota shows diurnal oscillations that are synchronized by the host's circadian clock and feeding rhythms. Short-chain fatty acids (SCFAs) produced by the microbiota are possible synchronizers of peripheral circadian clocks. We aimed to investigate whether faecal SCFAs show a diurnal rhythm that regulates the rhythm of SCFA receptor expression (FFAR2/3, OLFR78, HCAR2) and SCFA-induced colonic contractility. The role of the circadian clock was studied in mice lacking the core clock gene Bmal1. Methods Mice were sacrificed at 4-hour intervals. Faecal SCFA concentrations and SCFA receptor expression were determined. The effect of increasing concentrations of a SCFA mix on electrical field-induced neural responses in colon strips was measured isometrically. Results Diurnal fluctuations in faecal SCFA concentrations (peak 4 hours after lights on) were observed that were in phase with the rhythm of Ffar2/3 expression in the colonic muscle layer. Olfr78 expression was not diurnal and Hcar2 was not detectable. The inhibitory effect of a SCFA mix on neural contractions in colonic smooth muscle strips showed a diurnal rhythm and oscillated in phase with faecal SCFA concentrations and Ffar2/3 expression. In contrast, neither excitatory neural responses nor acetylcholine-induced smooth muscle contractions showed a diurnal rhythm. In Bmal1(-/-) mice, no fluctuations in faecal SCFA levels, Ffar3 expression and neural responses to SCFAs were observed. Conclusion Diurnal microbial SCFA levels regulate the rhythm of Ffar3 expression in the colonic myenteric plexus, which causes rhythmicity in SCFA-induced colonic motility. Deletion of Bmal1 abolishes rhythmicity of SCFA levels and their downstream effects.
机译:瞄准Microbiota显示由主昼夜昼夜时钟和喂养节奏同步的昼夜振荡。 Microbiota生产的短链脂肪酸(SCFA)是外围昼夜周边时钟的同步器。我们旨在调查粪便SCFA是否显示昼夜节律,该节奏调节SCFA受体表达的节奏(FFAR2 / 3,OLFR78,HCAR2)和SCFA诱导的结肠收缩性。在缺乏核心钟表基因BMAL1的小鼠中研究了昼夜节点的作用。方法以4小时间隔处死小鼠。确定粪便SCFA浓度和SCFA受体表达。在空常上测量增加SCFA混合物对电场诱导的电场诱导的神经反应的效果。结果观察到粪便SCFA浓度的昼夜波动(灯光后4小时),其与结肠肌层中FFAR2 / 3表达的节奏相位。 OLFR78表达不是昼夜,HCAR2无法检测到。 SCFA混合物在结肠平滑肌条中对神经收缩的抑制作用显示出昼夜节律和粪便SCFA浓度和FFAR2 / 3表达相位振荡。相比之下,兴奋性神经应答和乙酰胆碱诱导的平滑肌收缩都没有显示出昼夜节律。在BMA11( - / - )小鼠中,观察到粪便SCFA水平,FFAR3表达和对SCFA的神经反应没有波动。结论昼夜微生物SCA水平调节结肠神经丛中FFAR3表达的节奏,从而引起SCFA诱导的结肠运动性的节律性。 BMAL1的缺失废除了SCFA水平的节奏及其下游效应。

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