The role of the SLC6A3 3' UTR VNTR in nicotine effects on cognitive, affective, and motor function
Schroeder, Rebekka1; Reuter, Martin1; Fassbender, Kaja1; Plieger, Thomas1; Poulsen, Jessie5; Lui, Simon S. Y.2; Chan, Raymond C. K.3,4; Ettinger, Ulrich1
刊名PSYCHOPHARMACOLOGY
2021-12-02
通讯作者邮箱ulrich.ettinger@uni-bonn.de
页码19
关键词Nicotine DAT Smooth pursuit Inhibition Spontaneous blink rate Proactive inhibition Stop signal task Individual differences
ISSN号0033-3158
DOI10.1007/s00213-021-06028-x
产权排序4
文献子类综述
英文摘要

Rationale Nicotine has been widely studied for its pro-dopaminergic effects. However, at the behavioural level, past investigations have yielded heterogeneous results concerning effects on cognitive, affective, and motor outcomes, possibly linked to individual differences at the level of genetics. A candidate polymorphism is the 40-base-pair variable number of tandem repeats polymorphism (rs28363170) in the SLC6A3 gene coding for the dopamine transporter (DAT). The polymorphism has been associated with striatal DAT availability (9R-carriers > 10R-homozygotes), and 9R-carriers have been shown to react more strongly to dopamine agonistic pharmacological challenges than 10R-homozygotes. Objectives In this preregistered study, we hypothesized that 9R-carriers would be more responsive to nicotine due to genotype-related differences in DAT availability and resulting dopamine activity. Methods N=194 non-smokers were grouped according to their genotype (9R-carriers, 10R-homozygotes) and received either 2-mg nicotine or placebo gum in a between-subject design. Spontaneous blink rate (SBR) was obtained as an indirect measure of striatal dopamine activity and smooth pursuit, stop signal, simple choice and affective processing tasks were carried out in randomized order. Results Reaction times were decreased under nicotine compared to placebo in the simple choice and stop signal tasks, but nicotine and genotype had no effects on any of the other task outcomes. Conditional process analyses testing the mediating effect of SBR on performance and how this is affected by genotype yielded no significant results. Conclusions Overall, we could not confirm our main hypothesis. Individual differences in nicotine response could not be explained by rs28363170 genotype.

收录类别SCI
资助项目Projekt DEAL ; German Academic Scholarship Foundation ; Innovation Fund Denmark[7038-00043B] ; CAS Key Laboratory of Mental Health, Institute of Psychology
WOS关键词STRIATAL DOPAMINE TRANSPORTER ; EYE BLINK RATE ; RESPONSE-INHIBITION ; INDIVIDUAL-DIFFERENCES ; TRANSDERMAL NICOTINE ; AFFECTIVE EXPERIENCE ; TOBACCO SMOKING ; SCHIZOPHRENIA ; ATTENTION ; GENE
WOS研究方向Neurosciences & Neurology ; Pharmacology & Pharmacy ; Psychiatry
出版者SPRINGER
WOS记录号WOS:000725378600002
资助机构Projekt DEAL ; German Academic Scholarship Foundation ; Innovation Fund Denmark ; CAS Key Laboratory of Mental Health, Institute of Psychology
内容类型期刊论文
源URL[http://ir.psych.ac.cn/handle/311026/41276]  
专题心理研究所_中国科学院心理健康重点实验室
通讯作者Ettinger, Ulrich
作者单位1.Univ Bonn, Dept Psychol, Bonn, Germany
2.Univ Hong Kong, Hong Kong Special Adm Reg, Dept Psychiat, Hong Kong, Peoples R China
3.Inst Psychol, Neuropsychol & Appl Cognit Neurosci NACN Lab, CAS Key Lab Mental Hlth, Beijing, Peoples R China
4.Univ Chinese Acad Sci, Dept Psychol, Beijing, Peoples R China
5.Fertin Pharma AS, Nicotine Sci Ctr, Vejle, Denmark
推荐引用方式
GB/T 7714
Schroeder, Rebekka,Reuter, Martin,Fassbender, Kaja,et al. The role of the SLC6A3 3' UTR VNTR in nicotine effects on cognitive, affective, and motor function[J]. PSYCHOPHARMACOLOGY,2021:19.
APA Schroeder, Rebekka.,Reuter, Martin.,Fassbender, Kaja.,Plieger, Thomas.,Poulsen, Jessie.,...&Ettinger, Ulrich.(2021).The role of the SLC6A3 3' UTR VNTR in nicotine effects on cognitive, affective, and motor function.PSYCHOPHARMACOLOGY,19.
MLA Schroeder, Rebekka,et al."The role of the SLC6A3 3' UTR VNTR in nicotine effects on cognitive, affective, and motor function".PSYCHOPHARMACOLOGY (2021):19.
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