Department of Physiology, Northwestern University Feinberg School of Medicine, Chicago, Illinois 60611, USA.
J Biol Chem. 2012 Oct 19;287(43):35964-74. doi: 10.1074/jbc.M112.363358. Epub 2012 Sep 4.
The dendritic field of a neuron, which is determined by both dendritic architecture and synaptic strength, defines the synaptic input of a cell. Once established, a neuron's dendritic field is thought to remain relatively stable throughout a cell's lifetime. Perturbations in a dendritic structure or excitatory tone of a cell and thus its dendritic field are cellular alterations thought to be correlated with a number of psychiatric disorders. Although several proteins are known to regulate the development of dendritic arborization, much less is known about the mechanisms that maintain dendritic morphology and synaptic strength. In this study, we find that afadin, a component of N-cadherin·β-catenin·α-N-catenin adhesion complexes, is required for the maintenance of established dendritic arborization and synapse number. We further demonstrate that afadin directly interacts with AMPA receptors and that loss of this protein reduces the surface expression of GluA1- and GluA2-AMPA receptor subunits. Collectively, these data suggest that afadin is required for the maintenance of dendritic structure and excitatory tone.
神经元的树突场由树突结构和突触强度共同决定,它决定了一个细胞的突触输入。一旦建立,神经元的树突场在细胞的整个生命周期中被认为相对稳定。树突结构或细胞的兴奋性的改变,也就是其树突场的改变,被认为与许多精神疾病有关。虽然有几种蛋白质被认为可以调节树突分支的发育,但对于维持树突形态和突触强度的机制知之甚少。在这项研究中,我们发现粘连蛋白 afadin 是 N-钙黏蛋白-β-连环蛋白-α-连环蛋白黏附复合物的一个组成部分,它对于维持已建立的树突分支和突触数量是必需的。我们进一步证明,afadin 直接与 AMPA 受体相互作用,而这种蛋白质的缺失会减少 GluA1 和 GluA2-AMPA 受体亚基的表面表达。总的来说,这些数据表明 afadin 对于维持树突结构和兴奋性是必需的。
