Desai Shreya, Zundel Clara G, Evanski Julia M, Gowatch Leah C, Bhogal Amanpreet, Ely Samantha, Carpenter Carmen, Shampine MacKenna, O'Mara Emilie, Rabinak Christine A, Marusak Hilary A
Dept. of Psychiatry and Behavioral Neurosciences, Wayne State University School of Medicine, USA.
Dept. of Psychiatry and Behavioral Neurosciences, Wayne State University School of Medicine, USA; Dept. of Pharmacy Practice, Wayne State University, USA.
Behav Brain Res. 2024 Apr 12;463:114925. doi: 10.1016/j.bbr.2024.114925. Epub 2024 Feb 27.
The endocannabinoid system modulates neural activity throughout the lifespan. In adults, neuroimaging studies link a common genetic variant in fatty acid amide hydrolase (FAAH C385A)-an enzyme that regulates endocannabinoid signaling-to reduced risk of anxiety and depression, and altered threat- and reward-related neural activity. However, limited research has investigated these associations during the transition into adolescence, a period of substantial neurodevelopment and increased psychopathology risk.
This study included FAAH genotype and longitudinal neuroimaging and neurobehavioral data from 4811 youth (46% female; 9-11 years at Baseline, 11-13 years at Year 2) from the Adolescent Brain Cognitive Development Study. Linear mixed models examined the effects of FAAH and the FAAH x time interaction on anxiety and depressive symptoms, amygdala reactivity to threatening faces, and nucleus accumbens (NAcc) response to happy faces during the emotional n-back task.
A significant main effect of FAAH on depressive symptoms was observed, such that depressive symptoms were lower across both timepoints in those with the AA genotype compared to both AC and CC genotypes (p's<0.05). There were no significant FAAH x time interactions for anxiety, depression, or neural responses (p's>0.05). Additionally, there were no main effects of FAAH on anxiety or neural responses (p's>0.05).
Our findings add to emerging evidence linking the FAAH C385A variant to lower risk of psychopathology, and extend these findings to a developmental sample. In particular, we found lower depressive symptoms in FAAH AA genotypes compared to AC and CC genotypes. Future research is needed to characterize the role of the FAAH variant and the eCB system more broadly in neurodevelopment and psychiatric risk.
内源性大麻素系统在整个生命周期中调节神经活动。在成年人中,神经影像学研究将脂肪酸酰胺水解酶(FAAH C385A)中的一种常见基因变异——一种调节内源性大麻素信号传导的酶——与焦虑和抑郁风险降低以及与威胁和奖励相关的神经活动改变联系起来。然而,在向青春期过渡期间,这一时期神经发育迅速且心理病理学风险增加,对此类关联的研究有限。
本研究纳入了来自青少年大脑认知发展研究的4811名青少年(46%为女性;基线时9 - 11岁,第2年时11 - 13岁)的FAAH基因型以及纵向神经影像学和神经行为数据。线性混合模型研究了FAAH以及FAAH×时间交互作用对焦虑和抑郁症状、杏仁核对威胁性面孔的反应性以及伏隔核(NAcc)在情绪n-back任务中对开心面孔的反应的影响。
观察到FAAH对抑郁症状有显著的主效应,即与AC和CC基因型相比,AA基因型个体在两个时间点的抑郁症状均较低(p值<0.05)。在焦虑、抑郁或神经反应方面,未观察到显著的FAAH×时间交互作用(p值>0.05)。此外,FAAH对焦虑或神经反应没有主效应(p值>0.05)。
我们的研究结果进一步证明了FAAH C385A变异与较低的心理病理学风险之间的联系,并将这些发现扩展到了一个发育样本中。特别是,我们发现与AC和CC基因型相比,FAAH AA基因型个体的抑郁症状较低。未来需要进一步研究以更全面地描述FAAH变异和内源性大麻素系统在神经发育和精神疾病风险中的作用。
