Iowa Neuroscience Institute, The University of Iowa, Iowa City, Iowa 52242.
Department of Biology, The University of Iowa, Iowa City, Iowa 52242.
J Neurosci. 2023 Feb 8;43(6):918-935. doi: 10.1523/JNEUROSCI.0729-22.2022. Epub 2023 Jan 5.
The establishment of a functional cerebral cortex depends on the proper execution of multiple developmental steps, culminating in dendritic and axonal outgrowth and the formation and maturation of synaptic connections. Dysregulation of these processes can result in improper neuronal connectivity, including that associated with various neurodevelopmental disorders. The γ-Protocadherins (γ-Pcdhs), a family of 22 distinct cell adhesion molecules that share a C-terminal cytoplasmic domain, are involved in multiple aspects of neurodevelopment including neuronal survival, dendrite arborization, and synapse development. The extent to which individual γ-Pcdh family members play unique versus common roles remains unclear. We demonstrated previously that the γ-Pcdh-C3 isoform (γC3), via its unique "variable" cytoplasmic domain (VCD), interacts in cultured cells with Axin1, a Wnt-pathway scaffold protein that regulates the differentiation and morphology of neurons. Here, we confirm that γC3 and Axin1 interact in the cortex and show that both male and female mice specifically lacking γC3 exhibit disrupted Axin1 localization to synaptic fractions, without obvious changes in dendritic spine density or morphology. However, both male and female γC3 knock-out mice exhibit severely decreased dendritic complexity of cortical pyramidal neurons that is not observed in mouse lines lacking several other γ-Pcdh isoforms. Combining knock-out with rescue constructs in cultured cortical neurons pooled from both male and female mice, we show that γC3 promotes dendritic arborization through an Axin1-dependent mechanism mediated through its VCD. Together, these data identify a novel mechanism through which γC3 uniquely regulates the formation of cortical circuitry. The complexity of a neuron's dendritic arbor is critical for its function. We showed previously that the γ-Protocadherin (γ-Pcdh) family of 22 cell adhesion molecules promotes arborization during development; it remained unclear whether individual family members played unique roles. Here, we show that one γ-Pcdh isoform, γC3, interacts in the brain with Axin1, a scaffolding protein known to influence dendrite development. A CRISPR/Cas9-generated mutant mouse line lacking γC3 (but not lines lacking other γ-Pcdhs) exhibits severely reduced dendritic complexity of cerebral cortex neurons. Using cultured γC3 knock-out neurons and a variety of rescue constructs, we confirm that the γC3 cytoplasmic domain promotes arborization through an Axin1-dependent mechanism. Thus, γ-Pcdh isoforms are not interchangeable, but rather can play unique neurodevelopmental roles.
功能性大脑皮层的建立依赖于多个发育步骤的正确执行,最终导致树突和轴突的生长以及突触连接的形成和成熟。这些过程的失调可能导致神经元连接不当,包括与各种神经发育障碍相关的连接。γ-原钙黏蛋白(γ-Pcdh)是一个由 22 个不同的细胞黏附分子组成的家族,它们都具有一个共同的 C 端细胞质结构域,参与包括神经元存活、树突分支和突触发育在内的多个神经发育过程。目前尚不清楚个别γ-Pcdh 家族成员在发挥独特作用和共同作用方面的程度。我们之前曾证明,γ-Pcdh-C3 同种型(γC3)通过其独特的“可变”细胞质结构域(VCD)与 Axin1 在培养细胞中相互作用,Axin1 是一种 Wnt 通路支架蛋白,可调节神经元的分化和形态。在这里,我们证实了 γC3 和 Axin1 在皮质中相互作用,并表明雄性和雌性小鼠特异性缺失 γC3 会导致 Axin1 定位到突触部分的情况受到干扰,而树突棘密度或形态没有明显变化。然而,雄性和雌性 γC3 敲除小鼠表现出皮质锥体神经元树突复杂性严重降低,而在缺乏几种其他 γ-Pcdh 同种型的小鼠系中没有观察到这种情况。通过在来自雄性和雌性小鼠的培养皮质神经元中进行敲除与挽救构建体的组合,我们证明了 γC3 通过其 VCD 依赖的机制促进树突分支。总之,这些数据确定了一种新的机制,通过该机制,γC3 独特地调节皮质回路的形成。神经元树突的复杂性对于其功能至关重要。我们之前曾表明,22 种细胞黏附分子的γ-原钙黏蛋白(γ-Pcdh)家族在发育过程中促进树突分支;但尚不清楚个别家族成员是否发挥独特作用。在这里,我们表明一种γ-Pcdh 同种型γC3 在大脑中与 Axin1 相互作用,Axin1 是一种已知影响树突发育的支架蛋白。使用 CRISPR/Cas9 生成的突变小鼠系(但不是缺乏其他 γ-Pcdhs 的系)缺失 γC3 会导致大脑皮层神经元的树突复杂性严重降低。使用培养的 γC3 敲除神经元和各种挽救构建体,我们证实 γC3 细胞质结构域通过 Axin1 依赖的机制促进树突分支。因此,γ-Pcdh 同种型不是可互换的,而是可以发挥独特的神经发育作用。
