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Nasal versus temporal illumination of the human retina: Effects on core body temperature, melatonin, and circadian phase

机译:人体视网膜的鼻腔照明与时间照明:对核心体温,褪黑激素和昼夜节律的影响

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The mammalian retina contains both visual and circadian photoreceptors. In humans, nocturnal stimulation of the latter receptors leads to melatonin suppression, which might cause reduced nighttime sleepiness. Melatonin suppression is maximal when the nasal part of the retina is illuminated. Whether circadian phase shifting in humans is due to the same photoreceptors is not known. The authors explore whether phase shifts and melatonin suppression depend on the same retinal area. Twelve healthy subjects participated in a within-subjects design and received all of 3 light conditions-1) 10 lux of dim light on the whole retina, 2) 100 lux of ocular light on the nasal part of the retina, and 3) 100 lux of ocular light on the temporal part of the retina-on separate nights in random order. In all 3 conditions, pupils were dilated before and during light exposure. The protocol consisted of an adaptation night followed by a 23-h period of sustained wakefulness, during which a 4-h light pulse was presented at a time when maximal phase delays were expected. Nasal illumination resulted in an immediate suppression of melatonin but had no effect on subjective sleepiness or core body temperature (CBT). Nasal illumination delayed the subsequent melatonin rhythm by 78 min, which is significantly (p = 0.016) more than the delay drift in the dim-light condition (38 min), but had no detectable phase-shifting effect on the CBT rhythm. Temporal illumination suppressed melatonin less than the nasal illumination and had no effect on subjective sleepiness and CBT. Temporal illumination delayed neither the melatonin rhythm nor the CBT rhythm. The data show that the suppression of melatonin does not necessarily result in a reduction of subjective sleepiness and an elevation of CBT. In addition, 100 lux of bright white light is strong enough to affect the photoreceptors responsible for the suppression of melatonin but not strong enough to have a significant effect on sleepiness and CBT. This may be due to the larger variability of the latter variables.
机译:哺乳动物的视网膜包含视觉和昼夜节律的感光体。在人类中,后一种受体的夜间刺激导致褪黑激素抑制,这可能导致夜间嗜睡减少。当视网膜的鼻部被照亮时,褪黑激素的抑制作用最大。尚不清楚人类的昼夜节律相移是否是由于相同的感光体引起的。作者探讨了相移和褪黑激素抑制是否依赖于同一视网膜区域。十二名健康受试者参与了受试者内部设计,并接受了3种光照条件的全部条件:1)整个视网膜的光照为10 lux,2)视网膜鼻腔的光照为100 lux,3)光照为100 lux在视网膜的颞部以随机的顺序排列眼底光。在所有3种情况下,瞳孔在曝光之前和曝光期间都会散大。该协议包括一个适应之夜,之后是23小时的持续清醒,在此期间,在预期最大相位延迟的时间出现了4小时的光脉冲。鼻腔照明可立即抑制褪黑激素,但对主观嗜睡或核心体温(CBT)没有影响。鼻照明将随后的褪黑激素节律延迟了78分钟,这比暗光条件下的延迟漂移(38分钟)要大(p = 0.016),但对CBT节律没有可检测到的相移效应。时空照明对褪黑激素的抑制作用少于鼻腔照明,对主观嗜睡和CBT没有影响。时间照明既不延迟褪黑激素节律也不延迟CBT节律。数据表明,褪黑激素的抑制并不一定导致主观嗜睡的减少和CBT的升高。另外,100 lux的明亮白光强度足以影响负责褪黑激素抑制的感光体,但强度不足以对困倦和CBT产生显着影响。这可能是由于后一个变量的较大可变性。

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