Grant Leilah K, Cain Sean W, Chang Anne-Marie, Saxena Richa, Czeisler Charles A, Anderson Clare
Monash Institute of Cognitive and Clinical Neurosciences, School of Psychological Sciences, Monash University, Clayton, Victoria 3800, Australia.
Monash Institute of Cognitive and Clinical Neurosciences, School of Psychological Sciences, Monash University, Clayton, Victoria 3800, Australia; Sleep Health Institute and Division of Sleep and Circadian Disorders, Departments of Medicine and Neurology, Brigham and Women's Hospital, Boston, MA 02115, USA.
Behav Brain Res. 2018 Feb 15;338:51-55. doi: 10.1016/j.bbr.2017.09.025. Epub 2017 Sep 22.
Accumulating evidence points to a genetic contribution to explain inter-individual vulnerability to sleep deprivation. A functional polymorphism in the BDNF gene, which causes a valine (Val) to methionine (Met) amino acid substitution at Codon 66, has been associated with cognitive impairment, particularly in populations with impaired frontal functioning. We hypothesised that sleep deprivation, which affects frontal function, may lead to cognitive dysfunction in Met allele carriers. To examine this, we investigated, in different BDNF genotypes, the effects of sleep deprivation on cognitive flexibility, as measured by response inhibition using the Stroop Color Naming Task. Thirty healthy, adults of European ancestry, including 12 heterozygous Met allele carriers and 18 Val/Val homozygotes, underwent 30-h of extended wakefulness under constant routine conditions. A computerised Stroop task was administered every 2h. Error rate and reaction times increased with time awake for all individuals. Participants with the Val/Met genotype made more errors on incongruent trials after 20h awake. While Val/Met participants also took significantly longer to respond when inhibiting a prepotent response irrespective of time awake, this was particularly evident during the biological night. Our study shows that carriers of the BDNF Met allele are more vulnerable to the impact of prolonged wakefulness and the biological night on a critical component of executive function, as measured by response inhibition on the Stroop task.
越来越多的证据表明,基因在解释个体对睡眠剥夺的易感性方面发挥着作用。脑源性神经营养因子(BDNF)基因的一个功能性多态性,导致第66位密码子处缬氨酸(Val)到蛋氨酸(Met)的氨基酸替换,已与认知障碍相关,尤其是在额叶功能受损的人群中。我们假设,影响额叶功能的睡眠剥夺可能会导致Met等位基因携带者出现认知功能障碍。为了验证这一点,我们研究了不同BDNF基因型中,睡眠剥夺对认知灵活性的影响,认知灵活性通过使用斯特鲁普颜色命名任务进行反应抑制来衡量。30名健康的欧洲血统成年人,包括12名杂合Met等位基因携带者和18名Val/Val纯合子,在恒定日常条件下经历了30小时的持续清醒。每2小时进行一次计算机化的斯特鲁普任务。所有个体的错误率和反应时间都随着清醒时间的增加而增加。Val/Met基因型的参与者在清醒20小时后,在不一致试验中犯的错误更多。虽然Val/Met参与者在抑制优势反应时,无论清醒时间如何,反应时间也明显更长,但在生物夜间尤其明显。我们的研究表明,BDNF Met等位基因携带者更容易受到长时间清醒和生物夜间对执行功能关键组成部分的影响,执行功能通过斯特鲁普任务中的反应抑制来衡量。