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多巴胺通过激活对奖赏产生反应的杏仁核神经元来诱导恐惧消退。

Dopamine induces fear extinction by activating the reward-responding amygdala neurons.

作者信息

Zhang Xiangyu, Flick Katelyn, Rizzo Marianna, Pignatelli Michele, Tonegawa Susumu

机构信息

The Picower Institute for Learning and Memory, Department of Biology, Massachusetts Institute of Technology, Cambridge, MA 02139.

The Picower Institute for Learning and Memory, Department of Brain and Cognitive Sciences, Massachusetts Institute of Technology, Cambridge, MA 02139.

出版信息

Proc Natl Acad Sci U S A. 2025 May 6;122(18):e2501331122. doi: 10.1073/pnas.2501331122. Epub 2025 Apr 28.

Abstract

The extinction of conditioned fear responses is crucial for adaptive behavior, and its impairment is a hallmark of anxiety disorders such as posttraumatic stress disorder. Fear extinction takes place when animals form a new memory that suppresses the original fear memory. In the case of context-dependent fear memory, the new memory is formed within the reward-responding posterior subset of basolateral amygdala (BLA) that is genetically marked by neurons. These memory engram cells suppress the activity of the original fear-responding engram cells present in the anterior BLA, hence fear extinction. However, the neurological nature of the teaching signal that instructs the formation of fear extinction memory in the neurons is unknown. Here, we demonstrate that ventral tegmental area (VTA) dopaminergic signaling drives fear extinction in distinct BLA neuronal populations. We show that BLA fear and extinction neuronal populations receive topographically divergent inputs from VTA dopaminergic neurons via differentially expressed dopamine receptors. Fiber photometry recordings of dopaminergic activity in the BLA reveal that dopamine (DA) activity is time-locked to freezing cessation in BLA fear extinction neurons, but not BLA fear neurons. Furthermore, this dopaminergic activity in BLA fear extinction neurons correlates with extinction learning. Finally, using projection-specific optogenetic manipulation, we find that activation of the VTA DA projections to BLA reward and fear neurons accelerated or impaired fear extinction, respectively. Together, this work demonstrates that dopaminergic activity bidirectionally controls fear extinction by distinct patterns of activity at BLA fear and extinction neurons.

摘要

条件性恐惧反应的消退对于适应性行为至关重要,其受损是创伤后应激障碍等焦虑症的一个标志。当动物形成一种抑制原始恐惧记忆的新记忆时,恐惧消退就会发生。在情境依赖性恐惧记忆的情况下,新记忆是在基底外侧杏仁核(BLA)的奖励反应性后部亚群中形成的,该亚群由神经元进行基因标记。这些记忆印迹细胞抑制存在于前侧BLA中的原始恐惧反应印迹细胞的活动,从而实现恐惧消退。然而,指导神经元中恐惧消退记忆形成的教学信号的神经学本质尚不清楚。在这里,我们证明腹侧被盖区(VTA)多巴胺能信号在不同的BLA神经元群体中驱动恐惧消退。我们表明,BLA恐惧和消退神经元群体通过差异表达的多巴胺受体从VTA多巴胺能神经元接收拓扑学上不同的输入。对BLA中多巴胺能活动的光纤光度记录显示,多巴胺(DA)活动与BLA恐惧消退神经元中的僵立停止在时间上同步,但与BLA恐惧神经元不同步。此外,BLA恐惧消退神经元中的这种多巴胺能活动与消退学习相关。最后,使用投射特异性光遗传学操作,我们发现激活VTA向BLA奖励和恐惧神经元的多巴胺投射分别加速或损害了恐惧消退。总之,这项工作表明多巴胺能活动通过BLA恐惧和消退神经元的不同活动模式双向控制恐惧消退。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e0f3/12067255/b8ba9422dda0/pnas.2501331122fig01.jpg

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