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咖啡因的焦虑和警醒作用与 ADORA2A 和 ADORA1 多态性及习惯性咖啡因摄入量的关联。

Association of the anxiogenic and alerting effects of caffeine with ADORA2A and ADORA1 polymorphisms and habitual level of caffeine consumption.

机构信息

Department of Experimental Psychology, University of Bristol, Bristol, UK.

出版信息

Neuropsychopharmacology. 2010 Aug;35(9):1973-83. doi: 10.1038/npp.2010.71. Epub 2010 Jun 2.

Abstract

Caffeine, a widely consumed adenosine A(1) and A(2A) receptor antagonist, is valued as a psychostimulant, but it is also anxiogenic. An association between a variant within the ADORA2A gene (rs5751876) and caffeine-induced anxiety has been reported for individuals who habitually consume little caffeine. This study investigated whether this single nucleotide polymorphism (SNP) might also affect habitual caffeine intake, and whether habitual intake might moderate the anxiogenic effect of caffeine. Participants were 162 non-/low (NL) and 217 medium/high (MH) caffeine consumers. In a randomized, double-blind, parallel groups design they rated anxiety, alertness, and headache before and after 100 mg caffeine and again after another 150 mg caffeine given 90 min later, or after placebo on both occasions. Caffeine intake was prohibited for 16 h before the first dose of caffeine/placebo. Results showed greater susceptibility to caffeine-induced anxiety, but not lower habitual caffeine intake (indeed coffee intake was higher), in the rs5751876 TT genotype group, and a reduced anxiety response in MH vs NL participants irrespective of genotype. Apart from the almost completely linked ADORA2A SNP rs3761422, no other of eight ADORA2A and seven ADORA1 SNPs studied were found to be clearly associated with effects of caffeine on anxiety, alertness, or headache. Placebo administration in MH participants decreased alertness and increased headache. Caffeine did not increase alertness in NL participants. With frequent consumption, substantial tolerance develops to the anxiogenic effect of caffeine, even in genetically susceptible individuals, but no net benefit for alertness is gained, as caffeine abstinence reduces alertness and consumption merely returns it to baseline.

摘要

咖啡因是一种广泛使用的腺苷 A(1)和 A(2A)受体拮抗剂,被认为是一种精神兴奋剂,但它也具有焦虑作用。先前有研究报道,在习惯性摄入少量咖啡因的个体中,ADORA2A 基因(rs5751876)内的一个变体与咖啡因引起的焦虑之间存在关联。本研究旨在调查该单核苷酸多态性(SNP)是否也会影响习惯性咖啡因的摄入,以及习惯性摄入是否会调节咖啡因的焦虑作用。研究对象为 162 名非/低(NL)和 217 名中/高(MH)咖啡因消费者。采用随机、双盲、平行组设计,在饮用 100mg 咖啡因前后以及 90 分钟后再次饮用 150mg 咖啡因或两次饮用安慰剂之前,参与者对焦虑、警觉和头痛进行了评分。在首次服用咖啡因/安慰剂前 16 小时禁止摄入咖啡因。结果显示,rs5751876 TT 基因型组对咖啡因引起的焦虑更敏感,但习惯性咖啡因摄入(实际上咖啡摄入量更高)没有降低,而无论基因型如何,MH 参与者的焦虑反应均降低。除了几乎完全连锁的 ADORA2A SNP rs3761422 外,研究的 8 个 ADORA2A 和 7 个 ADORA1 SNPs 中没有其他 SNP 被发现与咖啡因对焦虑、警觉或头痛的影响明显相关。在 MH 参与者中,安慰剂的给药降低了警觉性并增加了头痛。NL 参与者中,咖啡因并没有增加警觉性。随着频繁摄入,即使在遗传易感个体中,对咖啡因的焦虑作用也会产生明显的耐受性,但警觉性并没有获得净收益,因为咖啡因戒断会降低警觉性,而摄入只会使其恢复到基线水平。

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