Literature DB >> 16272956

CYP2A6, MAOA, DBH, DRD4, and 5HT2A genotypes, smoking behaviour and cotinine levels in 1518 UK adolescents.

Shuwen Huang1, Derek G Cook, Lesley J Hinks, Xiao-He Chen, Shu Ye, Julie A Gilg, Martin J Jarvis, Peter H Whincup, Ian N M Day.   

Abstract

OBJECTIVES: Smoking is a major cause of death and often initiates in adolescence. Mutations in CYP2A6 slow metabolism of nicotine to cotinine. Haploinsufficiency in adults is associated with lower cigarette consumption, lower cotinine level and higher quit rates. Other genes are also implicated in smoking behaviour. We explored smoking behaviour and cotinine levels in relation to genotypes in adolescents.
METHODS: 1518 subjects from the Ten Towns Heart Health Study were genotyped for CYP2A6 alleles *1A, *1B, *2, *4, *5, *9 and *12 to classify predicted nicotine metabolism rate. DBH(rs77905), MAOA(rs1801291+VNTR), DRD4(VNTR) and 5HT2A(rs6313) were also studied. Smoking status was established by questionnaire and salivary cotinine measurement at 13-15 and 18 years.
RESULTS: No significant associations were identified for DBH, MAOA, DRD4 and 5HT2A markers, with smoking status or cotinine level at either age. At age 18, haploinsufficiency (HI) for CYP2A6 was associated with a higher odds of being a current smoker compared with the *1B carriers (WT1B) (OR = 2.23 (1.16, 4.27) for current versus ex); *1A homozygotes (WT1A) were also at slightly higher risk (OR = 1.44 (1.01, 2.06)). Partial haploinsufficiency (PHI) was not associated with being a current smoker. There were no significant associations at age 13-15. PHI and HI were associated with higher cotinine levels amongst smokers at both 13-15 and at 18 years compared with WT1B and WT1A groups.
CONCLUSIONS: CYP2A6 haploinsufficiency increases likelihood of continuing smoking in teenagers. We hypothesize an explanatory 'occupancy' model to explain why haploinsufficiency results in faster progression to nicotine dependence, but lower subsequent consumption.

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Year:  2005        PMID: 16272956     DOI: 10.1097/01213011-200512000-00002

Source DB:  PubMed          Journal:  Pharmacogenet Genomics        ISSN: 1744-6872            Impact factor:   2.089


  22 in total

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2.  Effects of nicotine deprivation and replacement on BOLD-fMRI response to smoking cues as a function of DRD4 VNTR genotype.

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3.  Smoking, smoking cessation, and risk of cardiovascular disease.

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Review 4.  Genetics and smoking behavior.

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5.  DRD4 VNTR polymorphism is associated with transient fMRI-BOLD responses to smoking cues.

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Review 6.  Incorporating the family as a critical context in genetic studies of children: implications for understanding pathways to risky behavior and substance use.

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7.  Nicotine metabolism and addiction among adolescent smokers.

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8.  Associations of CYP2A6 genotype with smoking behaviors in southern China.

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9.  CYP2A6 Longitudinal Effects in Young Smokers.

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Review 10.  Constitutional mechanisms of vulnerability and resilience to nicotine dependence.

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