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海洛因使用者冒险行为增加与脑源性神经营养因子 Val66Met 多态性及血清脑源性神经营养因子水平降低相关。

Increased Risk-Taking Behaviour and Brain-Derived Neurotrophic Factor Val66Met Polymorphism Correlates to Decreased Serum Brain-Derived Neurotrophic Factor Level in Heroin Users.

机构信息

University of Rijeka, Faculty of Medicine, Rijeka, Croatia.

University of Primorska, Faculty of Health Sciences, Izola, Slovenia.

出版信息

Eur Addict Res. 2018;24(4):189-200. doi: 10.1159/000492582. Epub 2018 Aug 22.

Abstract

BACKGROUND

This study has examined the relationships and interactions between serum brain-derived neurotrophic factor (BDNF) levels, BDNF Val66Met polymorphism and self-reported risk-taking behaviour in individuals with a history of heroin use undergoing outpatient treatment in comparison to healthy individuals.

METHODS

We enrolled 167 heroin users and 86 healthy subjects and examined serum BDNF levels, Val66Met polymorphism, and personal characteristics using Connor Davidson Resilience Scale, Risk-taking (RT) propensity questionnaire, and Personality Assessment Inventory.

RESULTS

Heroin users had significantly higher serum BDNF levels than controls. In addition, serum BDNF levels were significantly higher in Val/Val carriers than in Met/Val or Met/Met in all recruited subjects. Furthermore, a stepwise multiple regression analysis of serum BDNF levels as a dependent variable with related factors showed that in heroin users, Alcohol Use Disorder Identification Test score, anxiety and RT score were found as independent contributors to serum BDNF levels. When performing gene-environment interaction it was additionally found that heroin users with self-reported high risk-taking behaviour had significantly lower levels of serum BDNF among heroin users with the Met allele.

CONCLUSIONS

These results indicate that genetic variant Met66 decreased the serum BDNF levels in combination with self-reported risk-taking propensity among heroin users. If results of future work confirm the influence of this combined effect between neurotrophic genotype and risk-taking behaviour, 66Met carriers might require higher levels of intervention to overcome their drug use pattern and risky behaviour.

摘要

背景

本研究考察了血清脑源性神经营养因子(BDNF)水平、BDNF Val66Met 多态性与有海洛因使用史的门诊治疗个体中报告的风险行为之间的关系和相互作用,并与健康个体进行了比较。

方法

我们招募了 167 名海洛因使用者和 86 名健康对照者,并使用 Connor-Davidson 韧性量表、风险倾向问卷和人格评估量表检查了血清 BDNF 水平、Val66Met 多态性和个人特征。

结果

海洛因使用者的血清 BDNF 水平明显高于对照组。此外,在所有入组的受试者中,Val/Val 携带者的血清 BDNF 水平明显高于 Met/Val 或 Met/Met 携带者。此外,以血清 BDNF 水平为因变量的逐步多元回归分析显示,在海洛因使用者中,酒精使用障碍识别测试评分、焦虑和风险行为评分是血清 BDNF 水平的独立影响因素。当进行基因-环境相互作用分析时,还发现报告有高风险行为的海洛因使用者的血清 BDNF 水平明显低于携带 Met 等位基因的海洛因使用者。

结论

这些结果表明,遗传变异 Met66 与海洛因使用者的自我报告风险倾向相结合,降低了血清 BDNF 水平。如果未来的研究工作证实这种神经营养基因型和风险行为之间的综合效应的影响,那么 66Met 携带者可能需要更高水平的干预来克服他们的药物使用模式和风险行为。

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