首页> 美国卫生研究院文献>International Journal of Endocrinology >“Gut Microbiota-Circadian Clock Axis” in Deciphering the Mechanism Linking Early-Life Nutritional Environment and Abnormal Glucose Metabolism
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“Gut Microbiota-Circadian Clock Axis” in Deciphering the Mechanism Linking Early-Life Nutritional Environment and Abnormal Glucose Metabolism

机译:“肠道菌群昼夜节律轴”揭示了早期营养环境与异常葡萄糖代谢之间的联系机制

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摘要

The prevalence of diabetes mellitus (DM) has been increasing dramatically worldwide, but the pathogenesis is still unknown. A growing amount of evidence suggests that an abnormal developmental environment in early life increases the risk of developing metabolic diseases in adult life, which is referred to as the “metabolic memory” and the Developmental Origins of Health and Disease (DOHaD) hypothesis. The mechanism of “metabolic memory” has become a hot topic in the field of DM worldwide and could be a key to understanding the pathogenesis of DM. In recent years, several large cohort studies have shown that shift workers have a higher risk of developing type 2 diabetes mellitus (T2DM) and worse control of blood glucose levels. Furthermore, a maternal high-fat diet could lead to metabolic disorders and abnormal expression of clock genes and clock-controlled genes in offspring. Thus, disorders of circadian rhythm might play a pivotal role in glucose metabolic disturbances, especially in terms of early adverse nutritional environments and the development of metabolic diseases in later life. In addition, as a peripheral clock, the gut microbiota has its own circadian rhythm that fluctuates with periodic feeding and has been widely recognized for its significant role in metabolism. In light of the important roles of the gut microbiota and circadian clock in metabolic health and their interconnected regulatory relationship, we propose that the “gut microbiota-circadian clock axis” might be a novel and crucial mechanism to decipher “metabolic memory.” The “gut microbiota-circadian clock axis” is expected to facilitate the future development of a novel target for the prevention and intervention of diabetes during the early stage of life.
机译:在世界范围内,糖尿病(DM)的患病率急剧上升,但其发病机理仍未知。越来越多的证据表明,早年的异常发育环境会增加成年后患代谢性疾病的风险,这被称为“代谢记忆”和健康与疾病的发展起源(DOHaD)假说。 “代谢记忆”的机制已成为世界范围内DM领域的热门话题,并且可能是理解DM发病机理的关键。近年来,几项大型队列研究表明,轮班工人罹患2型糖尿病(T2DM)的风险较高,并且血糖水平控制较差。此外,孕妇高脂饮食可能导致后代代谢紊乱以及时钟基因和时钟控制基因的异常表达。因此,昼夜节律紊乱可能在葡萄糖代谢紊乱中起关键作用,尤其是在早期不利的营养环境和晚年代谢疾病的发展方面。另外,作为外围时钟,肠道菌群具有其自身的昼夜节律,该节律随着周期性进食而波动,并且由于其在新陈代谢中的重要作用而被广泛认可。鉴于肠道菌群和生物钟在代谢健康中的重要作用及其相互联系的调节关系,我们认为“肠道菌群-生物钟时钟轴”可能是破译“代谢记忆”的一种新颖且至关重要的机制。预计“肠道菌群生物钟”将促进生命早期阶段预防和干预糖尿病的新靶标的未来发展。

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