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Prefronto-subcortical imbalance characterizes poor decision-making: neurochemical and neural functional evidences in rats

机译:前额皮层下皮层失衡是不良决策的特征:大鼠的神经化学和神经功能证据

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A major challenge of decision-making research in recent years has been to develop models of poor decision-making to identify its neural bases. Toward this goal, we developed a Rat Gambling Task that discerns good and poor decision-makers in a complex and conflicting situation such as the human Iowa Gambling Task. Nothing is known about the role of the monoaminergic modulatory systems in shaping these phenotypes. Moreover, functional and temporal contributions of brain areas during poor compared to good decision-making remains elusive. Good and poor decision-makers were identified in the Rat Gambling Task. We investigated neurobiological correlates of decision-making capacities in (1) dopamine and serotonin turnovers using post-mortem tissue measurements, (2) the neural circuits differentially recruited during decision-making within the prefronto-subcortical network using cellular Fos immunodetection. Imbalance in monoamine metabolism was revealed in poor decision-makers, i.e. a higher infralimbic vs. lower amygdala serotonergic metabolism. Moreover, good decision-making recruited a wide prefronto-subcortical network but once good choices had been made, a disengagement of key prefrontal areas (insular and infralimbic cortices notably) and the amygdala was observed. By contrast, poor decision-making was associated with a strikingly low recruitment of the prefronto-subcortical network, together with sustained amygdala activity. Our results identify two complementary neurobiological substrates characterizing poor decision-makers: imbalanced monoaminergic systems at rest, congruent with their previously identified complex behavioral phenotype, and an aberrant low recruitment of key brain areas for executive functions and affective valence during the process of decision-making. These biomarkers could sustain vulnerability to developing poor decision-making related disorders.
机译:近年来,决策研究的主要挑战是开发决策能力差的模型以识别其神经基础。为了实现这一目标,我们开发了一项“老鼠赌博”任务,该任务可以识别复杂和冲突情况下的好坏决策者,例如人类爱荷华州的赌博任务。关于单胺能调节系统在塑造这些表型中的作用还一无所知。而且,与良好的决策相比,在贫困时期大脑区域的功能和时间贡献仍然难以捉摸。在老鼠赌博任务中确定了好的和坏的决策者。我们调查了死后组织测量中(1)多巴胺和5-羟色胺更新的决策能力与神经生物学的相关性,(2)在前额叶下皮层网络中使用细胞Fos免疫检测在决策过程中差异性募集的神经回路。在不良的决策者中发现了单胺代谢的失衡,即较高的下肢抵抗力与较低的杏仁核血清素能代谢。此外,良好的决策可以招募到广泛的额前皮下皮层网络,但是一旦做出了明智的选择,关键的额前皮区域(尤其是中枢皮层和下缘皮层)就会脱离,并观察到杏仁核。相比之下,糟糕的决策与前额皮下皮层网络的招募非常少以及持续的杏仁核活动有关。我们的结果确定了两个互补的神经生物学底物,这些底物是决策者的特征:静止时的单胺能系统失衡,与其先前确定的复杂行为表型一致,以及决策过程中关键大脑区域的异常低的执行功能和情感价的募集。这些生物标记物可以维持发展为与决策相关的不良疾病的脆弱性。

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