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早期生活逆境选择性地中断雄性小鼠背外侧纹状体神经元的树突分化。

Early-life adversity selectively interrupts the dendritic differentiation of dorsolateral striatal neurons in male mice.

机构信息

Department of Human Anatomy, School of Basic Medical Sciences, Yangtze University, Hubei, 434023, China.

Jingzhou Central Hospital, The Second Clinical Medical College, Yangtze University, Hubei, 434020, China.

出版信息

Brain Struct Funct. 2021 Mar;226(2):397-414. doi: 10.1007/s00429-020-02183-7. Epub 2021 Jan 2.

Abstract

The effects of early-life adversity (ELA) on dendritic differentiation of striatal neurons were investigated in the dorsal striatum including the dorsomedial striatum and dorsolateral striatum (DMS and DLS, respectively). An animal model of ELA was created by changing the growth environment of newborn mouse pups by giving limited bedding and nesting materials from postnatal day 2 to day 9 (P2-P9). One week after the stress paradigm (P16), the dendritic branches and spines of striatal spiny neurons as well as the synapses represented by postsynaptic density protein-95 (PSD-95) in DMS and DLS were stereologically analyzed. Adverse experience in early life selectively affected the spiny neurons in DLS, leading to abundant proximal dendritic branches and an increased number of filopodia-like protrusions, but a reduced number of dendritic spines. The selective effects of stress on neurons in DLS were further identified by reduced expression of PSD-95, including a reduced optical density of PSD-95 immunoreactivity and fewer individual PSD-95 immunoreactive synapses in this region. Notably, stress in early life affected either D1 or D2 dopamine receptor-expressing DLS neurons. These findings suggest that adverse early-life experience delayed the maturation of dendritic spines on neurons in the dorsolateral striatum. Altered dendritic differentiation provoked by stress in early life may contribute critically to the formation of proper neuronal circuits in the dorsal striatum and, therefore, affect striatum-dependent habitual behavior and emotional function later in life.

摘要

早期生活逆境 (ELA) 对纹状体神经元树突分化的影响在包括背侧纹状体在内的背侧纹状体中进行了研究,其中包括背内侧纹状体和背外侧纹状体(分别为 DMS 和 DLS)。通过在新生小鼠幼仔出生后第 2 天至第 9 天(P2-P9)给予有限的被褥和筑巢材料来改变其生长环境,从而创建 ELA 动物模型。应激范式后 1 周(P16),对 DMS 和 DLS 中的纹状体棘突神经元的树突分支和棘突以及突触后密度蛋白-95(PSD-95)代表的突触进行了立体学分析。早期生活中的逆境经历选择性地影响 DLS 中的棘突神经元,导致丰富的近端树突分支和增加的丝状伪足样突起数量,但树突棘数量减少。通过 PSD-95 表达减少,进一步确定了应激对 DLS 神经元的选择性影响,包括该区域 PSD-95 免疫反应的光密度降低和个体 PSD-95 免疫反应性突触减少。值得注意的是,早期生活中的应激会影响 DLS 中表达 D1 或 D2 多巴胺受体的神经元。这些发现表明,不良的早期生活经历会延迟背外侧纹状体神经元树突棘的成熟。早期生活应激引起的树突分化改变可能会对背侧纹状体中适当神经元回路的形成产生至关重要的影响,从而影响纹状体依赖的习惯性行为和以后的情绪功能。

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