Cajal Institute, Translational Neuroscience Department, Consejo Superior de Investigaciones Científicas, 28002 Madrid, Spain.
Institute of Molecular Biology, Consejo Superior de Investigaciones Científicas, 08028 Barcelona, Spain.
J Neurosci. 2021 Aug 11;41(32):6836-6849. doi: 10.1523/JNEUROSCI.2619-20.2021. Epub 2021 Jul 1.
Adult neural plasticity is an important and intriguing phenomenon in the brain, and adult hippocampal neurogenesis is directly involved in modulating neural plasticity by mechanisms that are only partially understood. We have performed gain-of-function and loss-of-function experiments to study Smad2, a transcription factor selected from genes that are demethylated after exercise through the analysis of an array of physical activity-induced factors, and their corresponding gene expression, and an efficient inducer of plasticity. In these studies, changes in cell number and morphology were analyzed in the hippocampal dentate gyrus (cell proliferation and survival, including regional distribution, and structural maturation/differentiation, including arborization, dendritic spines, and neurotransmitter-specific vesicles) of sedentary male mice, after evaluation in a battery of behavioral tests. As a result, we reveal a role for Smad2 in the balance of proliferation versus maturation of differentiating immature cells (Smad2 silencing increases both the proliferation and survival of cycling cells in the dentate granule cell layer), and in the plasticity of both newborn and mature neurons in mice (by decreasing dendritic arborization and dendritic spine number). Moreover, Smad2 silencing specifically compromises spatial learning in mice (through impairments of spatial tasks acquisition both in long-term learning and working memory). These data suggest that Smad2 participates in adult neural plasticity by influencing the proliferation and maturation of dentate gyrus neurons. Smad2 is one of the main components of the transforming growth factor-β (TGF-β) pathway. The commitment of cell fate in the nervous system is tightly coordinated by SMAD2 signaling, as are further differentiation steps (e.g., dendrite and axon growth, myelination, and synapse formation). However, there are no studies that have directly evaluated the role of gene in hippocampus of adult animals. Modulation of these parameters in the adult hippocampus can affect hippocampal-dependent behaviors, which may shed light on the mechanisms that regulate adult neurogenesis and behavior. We demonstrate here a role for Smad2 in the maturation of differentiating immature cells and in the plasticity of mature neurons. Moreover, Smad2 silencing specifically compromises the spatial learning abilities of adult male mice.
成人神经可塑性是大脑中的一个重要而有趣的现象,而成人海马神经发生则通过部分尚未完全理解的机制直接参与调节神经可塑性。我们通过过表达和基因敲低实验研究了 Smad2,Smad2 是从运动后去甲基化的基因中筛选出来的转录因子,通过分析一系列与体力活动相关的因素及其相应的基因表达,Smad2 是一种有效的可塑性诱导剂。在这些研究中,我们评估了一系列行为测试后,分析了久坐雄性小鼠海马齿状回(细胞增殖和存活,包括区域分布,以及结构成熟/分化,包括分支、树突棘和神经递质特异性囊泡)中细胞数量和形态的变化。结果表明,Smad2 在调节分化中的未成熟细胞的增殖与成熟平衡中起作用(Smad2 沉默增加了齿状颗粒细胞层中循环细胞的增殖和存活),以及在成年小鼠中新生和成熟神经元的可塑性中起作用(通过减少树突分支和树突棘数量)。此外,Smad2 沉默特异性损害了小鼠的空间学习能力(通过损害长期学习和工作记忆中的空间任务获得)。这些数据表明,Smad2 通过影响海马齿状回神经元的增殖和成熟参与成人神经可塑性。Smad2 是转化生长因子-β(TGF-β)途径的主要成分之一。SMAD2 信号在神经系统中严格协调细胞命运的决定,进一步的分化步骤(例如,树突和轴突生长、髓鞘形成和突触形成)也是如此。然而,目前还没有研究直接评估该基因在成年动物海马中的作用。在成年海马中调节这些参数可以影响海马依赖的行为,这可能揭示调节成年神经发生和行为的机制。我们在这里证明了 Smad2 在分化中的未成熟细胞的成熟和成熟神经元的可塑性中的作用。此外,Smad2 沉默特异性损害了成年雄性小鼠的空间学习能力。
