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唾液中的α-淀粉酶水平与长时间清醒时的神经行为警觉性有关,但与模拟夜班工作无关。

Salivary levels of alpha-amylase are associated with neurobehavioral alertness during extended wakefulness, but not simulated night-shift work.

机构信息

School of Pharmacy and Medical Sciences, University of South Australia, Adelaide, Australia.

Sleep and Chronobiology Laboratory, Behaviour-Brain-Body Research Centre, University of South Australia, Adelaide, Australia.

出版信息

Physiol Behav. 2019 May 15;204:1-9. doi: 10.1016/j.physbeh.2019.02.004. Epub 2019 Feb 5.

Abstract

Sleep loss is one of the most common causes of accidents and errors in operational environments. Currently, no single method satisfies all of the requisite criteria of an effective system for assessing the risk of injury prior to safety being compromised. Research has concentrated towards the development of a biomarker for individualized assessment of sleepiness-related deficits in neurobehavioral alertness, with salivary alpha-amylase (sAA) recently reported as a potential biomarker during acute total sleep deprivation. The present study extends on previous research by investigating the association between sAA and neurobehavioral alertness during simulated night-shift work, during individuals are required to work at night when biological processes are strongly promoting sleep and sleep during the day when endogenous processes are promoting wakefulness. In a laboratory-controlled environment, 10 healthy non-shift working males aged 24.7 ± 5.3 years (mean ± SD) underwent four consecutive nights of simulated night-shift work. Between 17:30-04:30 h participants provided saliva samples and completed a 3 min psychomotor vigilance test (PVT-B), 40 min simulated driving task, and 3 min digit symbol substitution test (DSST). Higher sAA levels were associated with faster response speed on the PVT-B, reduced lane variability on the simulated driving task, and improved information processing speed on the DSST during the first night-shift. There were no associations between sAA levels and performance outcomes during subsequent night-shifts. Findings indicate that the usability of sAA to assess the risk of neurobehavioral deficits during shift-work operations is limited. However, the robust circadian rhythm exhibited by sAA during the protocol of circadian misalignment suggests that sAA could serve as a potential circadian marker.

摘要

睡眠缺失是操作环境中事故和失误的最常见原因之一。目前,没有任何单一方法能满足评估伤害风险前的所有必要标准,这些方法需要安全无虞。研究集中于开发生物标志物,以对与睡眠相关的神经行为警觉性缺陷进行个体化评估,唾液α-淀粉酶(sAA)最近被报道为急性完全睡眠剥夺期间的潜在生物标志物。本研究通过调查 sAA 与模拟夜间轮班工作期间的神经行为警觉性之间的关联,进一步扩展了之前的研究,在模拟夜间轮班工作期间,个体需要在夜间工作,此时生物过程强烈促进睡眠,而在白天,内源性过程则促进清醒。在实验室控制环境中,10 名年龄 24.7±5.3 岁(均值±标准差)的健康非轮班工作男性连续 4 晚接受模拟夜间轮班工作。在 17:30-04:30 小时期间,参与者提供唾液样本并完成 3 分钟的精神运动警觉性测试(PVT-B)、40 分钟的模拟驾驶任务和 3 分钟的数字符号替代测试(DSST)。在第一个夜班期间,较高的 sAA 水平与 PVT-B 的反应速度加快、模拟驾驶任务中的车道变异性降低以及 DSST 的信息处理速度提高有关。在随后的夜班期间,sAA 水平与表现结果之间没有关联。研究结果表明,sAA 在评估轮班作业期间神经行为缺陷风险方面的可用性有限。然而,sAA 在昼夜节律失调方案中表现出的稳健昼夜节律表明,sAA 可能作为潜在的昼夜节律标志物。

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