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下丘脑多巴胺神经元通过持续的 cAMP 信号来激发交配行为。

Hypothalamic dopamine neurons motivate mating through persistent cAMP signalling.

机构信息

Division of Endocrinology, Diabetes and Metabolism, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA, USA.

Institute of Physiology, Department of Neurophysiology, Biocenter, Julius-Maximilians-University of Würzburg, Würzburg, Germany.

出版信息

Nature. 2021 Sep;597(7875):245-249. doi: 10.1038/s41586-021-03845-0. Epub 2021 Aug 25.

Abstract

Transient neuromodulation can have long-lasting effects on neural circuits and motivational states. Here we examine the dopaminergic mechanisms that underlie mating drive and its persistence in male mice. Brief investigation of females primes a male's interest to mate for tens of minutes, whereas a single successful mating triggers satiety that gradually recovers over days. We found that both processes are controlled by specialized anteroventral and preoptic periventricular (AVPV/PVpo) dopamine neurons in the hypothalamus. During the investigation of females, dopamine is transiently released in the medial preoptic area (MPOA)-an area that is critical for mating behaviours. Optogenetic stimulation of AVPV/PVpo dopamine axons in the MPOA recapitulates the priming effect of exposure to a female. Using optical and molecular methods for tracking and manipulating intracellular signalling, we show that this priming effect emerges from the accumulation of mating-related dopamine signals in the MPOA through the accrual of cyclic adenosine monophosphate levels and protein kinase A activity. Dopamine transients in the MPOA are abolished after a successful mating, which is likely to ensure abstinence. Consistent with this idea, the inhibition of AVPV/PVpo dopamine neurons selectively demotivates mating, whereas stimulating these neurons restores the motivation to mate after sexual satiety. We therefore conclude that the accumulation or suppression of signals from specialized dopamine neurons regulates mating behaviours across minutes and days.

摘要

短暂的神经调节可以对神经回路和动机状态产生持久的影响。在这里,我们研究了多巴胺能机制,这些机制是雄性小鼠交配驱动力及其持久性的基础。短暂的雌性调查会激发雄性交配的兴趣长达数十分钟,而单次成功交配会引发饱腹感,这种饱腹感会在数天内逐渐恢复。我们发现这两个过程都受到下丘脑特定的腹前核和视前正中核室旁核(AVPV/PVpo)多巴胺神经元的控制。在对雌性进行调查时,多巴胺会在中脑视前区(MPOA)短暂释放,这是交配行为的关键区域。光遗传刺激 MPOA 中的 AVPV/PVpo 多巴胺轴突可以再现暴露于雌性时的启动效应。通过使用光学和分子方法来跟踪和操纵细胞内信号,我们表明这种启动效应源自 MPOA 中与交配相关的多巴胺信号的积累,通过环磷酸腺苷水平和蛋白激酶 A 活性的积累。在成功交配后,MPOA 中的多巴胺瞬态被消除,这可能确保了禁欲。与这一观点一致的是,AVPV/PVpo 多巴胺神经元的抑制选择性地削弱了交配动机,而刺激这些神经元可以在性饱和后恢复交配的动机。因此,我们得出结论,特定多巴胺神经元的信号积累或抑制调节了几分钟到几天的交配行为。

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