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首页> 外文期刊>The Journal of Physiology >Recent observations on the regulation of fetal metabolism by glucose
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Recent observations on the regulation of fetal metabolism by glucose

机译:葡萄糖调节胎儿新陈代谢的最新观察

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Glucose is the principal energy substrate for the the fetus and is essential for normal fetal metabolism and growth. Fetal glucose metabolism is directly dependent on the fetal plasma glucose concentration. Fetal glucose utilization is augmented by insulin produced by the developing fetal pancreas in increasing amounts as gestation proceeds, which enhances glucose utilization among the insulin-sensitive tissues (skeletal muscle, liver, heart, adipose tissue) that incr ease in mass and thus glucose need during late gestation. Glucose-stimulated insulin secretion increases over gestation. Both insulin secretion and insulin action are affected by prevailing glucose concentrations and the amount and activity of tissue glucose transporters. In cases of intrauterine growth restriction (IUGR), fetal weight-specific tissue glucose uptake rates and glucose transporters are maintained or increased, while synthesis of amino acids into protein and corresponding insulin-IGF signal transduction proteins are decreased. These observations demonstrate the mixed phenotype of the IUGR fetus that includes enhanced glucose utilization capacity, but diminished protein synthesis and growth. Thus, the fetus has considerable capacity to adapt to changes in glucose supply by relatively common and understandable mechanisms that regulate fetal metabolism and growth and could underlie certain later life metabolic disorders such as insulin resistance, obesity and diabetes mellitus.
机译:葡萄糖是胎儿的主要能量底物,对于正常的胎儿代谢和生长至关重要。胎儿葡萄糖代谢直接取决于胎儿血浆葡萄糖浓度。胎儿的发育会随着妊娠的进行而增加胰岛素的量,从而增加胎儿的葡萄糖利用率,从而提高了胰岛素敏感组织(骨骼肌,肝脏,心脏,脂肪组织)的葡萄糖利用率,从而减轻了体重,从而增加了对葡萄糖的需求在妊娠后期。葡萄糖刺激的胰岛素分泌随妊娠而增加。胰岛素的分泌和胰岛素的作用都受到主要的葡萄糖浓度以及组织葡萄糖转运蛋白的量和活性的影响。在宫内生长受限(IUGR)的情况下,胎儿体重特异性组织的葡萄糖摄取率和葡萄糖转运蛋白得以维持或增加,而氨基酸合成蛋白质和相应的胰岛素-IGF信号转导蛋白质的合成减少。这些观察结果表明IUGR胎儿的混合表型包括增强的葡萄糖利用能力,但减少了蛋白质的合成和生长。因此,胎儿具有相当大的能力来通过调节胎儿新陈代谢和生长的相对普遍和可理解的机制来适应葡萄糖供应的变化,并且可能是某些晚年新陈代谢疾病的基础,例如胰岛素抵抗,肥胖症和糖尿病。

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