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Dysregulation of oxytocin and dopamine in the corticostriatal circuitry in bipolar II disorder

机译:双极II疾病中皮质棘菌电路中催产素和多巴胺的缺点

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The oxytocin (OXT) and dopamine systems synergistically facilitate striatal reactivity. Abnormal striatal activation has repeatedly been observed in patients with bipolar disorder (BD); however, such abnormality remains unclear in BD II. Here we aimed to investigate whether the corticostriatal connectivity was altered and the possible relationships among corticostriatal connectivity, OXT, and dopamine systems in BD II. Twenty-five BD II patients, as defined by the DSM-V, and 29 healthy controls (HC) were enrolled in this study. Plasma OXT was measured and striatal dopamine transporter (DAT) availability was assessed using [99mTc]TRODAT-1 single-photon emission computed tomography (SPECT). Brain network functional connectivity (FC) was measured during the resting-state using functional magnetic resonance imaging, and the dorsal caudate (DC) was selected as the seed region. The results showed that the OXT level was significantly lower in the BD II patients, while the striatal DAT availability was not significantly different between the BD II and HC groups. The BD II patients exhibited significantly lower FC between the DC and the executive control network (dorsolateral prefrontal, anterior cingulate cortex, and posterior parietal cortex) as compared with the HC. Only observed in HC, the DC-posterior parietal cortex FC was negatively correlated with the OXT level and striatal DAT availability. Our findings in the HC support a model in which the OXT and dopamine systems act in tandem to regulate corticostriatal circuitry, while the synergistic interaction was perturbed in BD II. Taken together, these results implied a maladaptive neuroplasticity in BD II.
机译:催产素(OXT)和多巴胺系统协同促进纹状体反应性。双相障碍(BD)患者反复观察到异常的纹状体活化;然而,这种异常在BD II中仍不清楚。在这里,我们旨在调查皮质棘腹连接是否改变和BD II中的皮质静脉连接,OXT和多巴胺系统中可能的关系。由DSM-V和29名健康对照(HC)定义的二十五名BD II患者均参与本研究。测量血浆OXT,使用[99MTC] TRODAT-1单光子发射计算断层扫描(SPECT)评估纹状体多巴胺转运蛋白(DAT)可用性。使用功能磁共振成像在静静脉状态下测量脑网络功能连接(FC),并选择背尾(DC)作为种子区域。结果表明,BD II患者的OXT水平显着较低,而BD II和HC组之间的纹状体可用性不会显着差异。与HC相比,BD II患者在DC和行政控制网络(背侧前额外,前部递送皮层和后部皮质)之间表现出显着降低的Fc。仅在HC中观察到,DC-Deparirioral Cortex Fc与OXT级别和尖端日期的可用性负相关。我们在HC中的发现支持一种模型,其中OXT和多巴胺系统在串联中起作用以调节皮质棘轮电路,而协同相互作用在BD II中扰乱。总之,这些结果暗示了BD II的不良神经塑性。

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