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Blood glucose concentration is unchanged during exposure to acute normobaric hypoxia in healthy humans

机译:在暴露于健康人类的急性正常源缺氧期间血糖浓度不变

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摘要

Normal blood [glucose] regulation is critical to support metabolism, particularly in contexts of metabolic stressors (e.g., exercise, high altitude hypoxia). Data regarding blood [glucose] regulation in hypoxia are inconclusive. We aimed to characterize blood [glucose] over 80 min following glucose ingestion during both normoxia and acute normobaric hypoxia. In a randomized cross‐over design, on two separate days, 28 healthy participants (16 females; 21.8 ± 1.6 years; BMI 22.8 ± 2.5 kg/m2) were randomly exposed to either NX (room air; fraction of inspired [FI]O2 ~0.21) or HX (FIO2 ~0.148) in a normobaric hypoxia chamber. Measured FIO2 and peripheral oxygen saturation were both lower at baseline in hypoxia (p < 0.001), which was maintained over 80 min, confirming the hypoxic intervention. Following a 10‐min baseline (BL) under both conditions, participants consumed a standardized glucose beverage (75 g, 296 ml) and blood [glucose] and physiological variables were measured at BL intermittently over 80 min. Blood [glucose] was measured from finger capillary samples via glucometer. Initial fasted blood [glucose] was not different between trials (NX:4.8 ± 0.4 vs. HX:4.9 ± 0.4 mmol/L; p = 0.47). Blood [glucose] was sampled every 10 min (absolute, delta, and percent change) following glucose ingestion over 80 min, and was not different between conditions (p > 0.77). In addition, mean, peak, and time‐to‐peak responses during the 80 min were not different between conditions (p > 0.14). There were also no sex differences in these blood [glucose] responses in hypoxia. We conclude that glucose regulation is unchanged in young, healthy participants with exposure to acute steady‐state normobaric hypoxia, likely due to counterbalancing mechanisms underlying blood [glucose] regulation in hypoxia.
机译:正常血液[葡萄糖]调节对于支持代谢至关重要,特别是在代谢应激源的背景下(例如,运动,高海拔缺氧)。关于缺氧中的血液调节的数据不确定。我们的目标是在常氧和急性正常的缺氧期间葡萄糖摄入后80分钟的血液[葡萄糖]。在一个随机的交叉设计中,在两个单独的日子,28个健康的参与者(16例女性; 21.8±1.6岁; BMI 22.8±2.5 kg / m 2)被随机暴露于NX(室内空间;一小部分启发[FI] O2 〜0.21)或NOMOBARIC缺氧室中的HX(FIO2〜0.148)。测量的FiO 2和外周氧饱和度在缺氧(P <0.001)中均较低,该基线保持超过80分钟,确认缺氧干预。在两种条件下,在两个条件下,参与者消耗标准化的葡萄糖饮料(75g,296ml)和血液β和生理变量,在BL间歇地超过80分钟。通过凝血仪从手指毛细管样品测量血液[葡萄糖]。初始禁食血液[葡萄糖]试验之间没有差异(NX:4.8±0.4与HX:4.9±0.4mmol / L; P = 0.47)。在葡萄糖摄入超过80分钟后每隔10分钟(绝对,δ和百分比)对血液进行取样,并且在条件下没有差异(p> 0.77)。另外,在80分钟内的平均值,峰值和峰值响应在条件(P> 0.14)之间没有差异。这些血液中也没有性差异[葡萄糖]在缺氧中的反应。我们得出结论,葡萄糖调节在患有暴露于急性稳态正常缺氧的年轻,健康参与者中不变,可能是由于血氧中血液β调节的抗衡机制造成的。

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