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Immunoglobulin-Like Receptors and Their Impact on Wiring of Brain Synapses
Annual Review of Genetics ( IF 8.7 ) Pub Date : 2018-11-26 00:00:00 , DOI: 10.1146/annurev-genet-120417-031513
Scott Cameron 1 , A Kimberley McAllister 1
Affiliation  

Synapse formation is mediated by a surprisingly large number and wide variety of genes encoding many different protein classes. One of the families increasingly implicated in synapse wiring is the immunoglobulin superfamily (IgSF). IgSF molecules are by definition any protein containing at least one Ig-like domain, making this family one of the most common protein classes encoded by the genome. Here, we review the emerging roles for IgSF molecules in synapse formation specifically in the vertebrate brain, focusing on examples from three classes of IgSF members: (a) cell adhesion molecules, (b) signaling molecules, and (c) immune molecules expressed in the brain. The critical roles for IgSF members in regulating synapse formation may explain their extensive involvement in neuropsychiatric and neurodevelopmental disorders. Solving the IgSF code for synapse formation may reveal multiple new targets for rescuing IgSF-mediated deficits in synapse formation and, eventually, new treatments for psychiatric disorders caused by altered IgSF-induced synapse wiring.

中文翻译:



免疫球蛋白样受体及其对脑突触接线的影响



突触的形成是由数量惊人、种类繁多的编码许多不同蛋白质类别的基因介导的。免疫球蛋白超家族(IgSF)是越来越多地与突触连接相关的家族之一。根据定义,IgSF 分子是含有至少一个 Ig 样结构域的任何蛋白质,使该家族成为基因组编码的最常见的蛋白质类别之一。在这里,我们回顾了 IgSF 分子在突触形成中的新作用,特别是在脊椎动物大脑中,重点关注三类 IgSF 成员的例子:( a ) 细胞粘附分子,( b ) 信号分子,和 ( c ) 在突触形成中表达的免疫分子大脑。 IgSF 成员在调节突触形成中的关键作用可能解释了它们广泛参与神经精神和神经发育障碍。解决突触形成的 IgSF 密码可能会揭示多个新靶标,以挽救 IgSF 介导的突触形成缺陷,并最终为因 IgSF 诱导的突触接线改变而引起的精神疾病提供新的治疗方法。

更新日期:2018-11-26
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