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A genetically modulated intrinsic cingulate circuit supports human nicotine addiction

机译:转基因的固有扣带回线支持人类尼古丁成瘾

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摘要

Whole-genome searches have identified nicotinic acetylcholine receptor α5-α3-β4 subunit gene variants that are associated with smoking. How genes support this addictive and high-risk behavior through their expression in the brain remains poorly understood. Here we show that a key α5 gene variant Asp398Asn is associated with a dorsal anterior cingulate–ventral striatum/extended amygdala circuit, such that the “risk allele” decreases the intrinsic resting functional connectivity strength in this circuit. Importantly, this effect is observed independently in nonsmokers and smokers, although the circuit strength distinguishes smokers from nonsmokers, predicts addiction severity in smokers, and is not secondary to smoking per se, thus representing a trait-like circuitry biomarker. This same circuit is further impaired in people with mental illnesses, who have the highest rate of smoking. Identifying where and how brain circuits link genes to smoking provides practical neural circuitry targets for new treatment development.
机译:全基因组搜索已确定了与吸烟有关的烟碱乙酰胆碱受体α5-α3-β4亚基基因变异。基因如何通过其在大脑中的表达来支持这种上瘾和高风险的行为仍然知之甚少。在这里,我们显示了一个关键的α5基因变异Asp398Asn与背前扣带回-腹侧纹状体/延伸杏仁核回路相关,因此“风险等位基因”降低了该回路中固有的静止功能连接强度。重要的是,这种效果在非吸烟者和吸烟者中是独立观察到的,尽管回路强度可以将吸烟者与非吸烟者区分开,可以预测吸烟者的成瘾严重程度,并且其本身并不是继发于吸烟的继发者,因此代表了性状样回路生物标记。在吸烟率最高的精神疾病患者中,同样的回路会进一步受损。确定大脑回路在何处以及如何将基因与吸烟联系起来,为开发新的治疗方法提供了实用的神经回路目标。

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