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Effects of methamphetamine abuse and serotonin transporter gene variants on aggression and emotion-processing neurocircuitry

机译:甲基苯丙胺滥用和5-羟色胺转运蛋白基因变异对攻击性和情绪处理神经回路的影响

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摘要

Individuals who abuse methamphetamine (MA) exhibit heightened aggression, but the neurobiological underpinnings are poorly understood. As variability in the serotonin transporter (SERT) gene can influence aggression, this study assessed possible contributions of this gene to MA-related aggression. In all, 53 MA-dependent and 47 control participants provided self-reports of aggression, and underwent functional magnetic resonance imaging while viewing pictures of faces. Participants were genotyped at two functional polymorphic loci in the SERT gene: the SERT-linked polymorphic region (SERT-LPR) and the intron 2 variable number tandem repeat polymorphism (STin2 VNTR); participants were then classified as having high or low risk for aggression according to individual SERT risk allele combinations. Comparison of SERT risk allele loads between groups showed no difference between MA-dependent and control participants. Comparison of self-report scores showed greater aggression in MA-dependent than control participants, and in high genetic risk than low-risk participants. Signal change in the amygdala was lower in high genetic risk than low-risk participants, but showed no main effect of MA abuse; however, signal change correlated negatively with MA use measures. Whole-brain differences in activation were observed between MA-dependent and control groups in the occipital and prefrontal cortex, and between genetic high- and low-risk groups in the occipital, fusiform, supramarginal and prefrontal cortex, with effects overlapping in a small region in the right ventrolateral prefrontal cortex. The findings suggest that the investigated SERT risk allele loads are comparable between MA-dependent and healthy individuals, and that MA and genetic risk influence aggression independently, with minimal overlap in associated neural substrates.
机译:滥用甲基苯丙胺(MA)的人表现出较高的攻击性,但对神经生物学的基础了解甚少。由于5-羟色胺转运蛋白(SERT)基因的变异性可以影响侵​​略性,因此本研究评估了该基因对MA相关侵袭的可能贡献。总共有53位依赖MA的参与者和47位对照参与者提供了攻击性的自我报告,并在查看面部图片时进行了功能磁共振成像。在SERT基因的两个功能性多态性位点对参与者进行基因分型:SERT连锁多态性区域(SERT-LPR)和内含子2可变数目串联重复多态性(STin2 VNTR);然后根据个体SERT风险等位基因组合将参加者分为侵略风险高或低。两组之间SERT风险等位基因负荷的比较显示,MA依赖性参与者和对照参与者之间没有差异。自我报告得分的比较显示,与MA相比,MA依赖者的攻击性更大,与低风险者相比,遗传风险更高。杏仁核的信号变化在高遗传风险中比低风险参与者低,但没有显示滥用MA的主要作用。但是,信号变化与MA使用措施负相关。在枕叶和额叶皮层的MA依赖组和对照组之间以及枕叶,梭形,上腹和额叶皮层的遗传性高风险和低风险组之间,观察到了全脑激活的差异。在右前外侧前额叶皮层。研究结果表明,所研究的SERT风险等位基因负荷在MA依赖者和健康个体之间是可比的,并且MA和遗传风险独立地影响攻击性,相关神经基质的重叠最小。

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