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在轴突细胞粘附分子L1与ERM家族成员之间鉴定出功能性结合相互作用。

Functional binding interaction identified between the axonal CAM L1 and members of the ERM family.

作者信息

Dickson Tracey C, Mintz C David, Benson Deanna L, Salton Stephen R J

机构信息

Fishberg Research Center for Neurobiology, The Mount Sinai School of Medicine, New York, NY 10029, USA.

出版信息

J Cell Biol. 2002 Jun 24;157(7):1105-12. doi: 10.1083/jcb.200111076. Epub 2002 Jun 17.

Abstract

A yeast two-hybrid library was screened using the cytoplasmic domain of the axonal cell adhesion molecule L1 to identify binding partners that may be involved in the regulation of L1 function. The intracellular domain of L1 bound to ezrin, a member of the ezrin, radixin, and moesin (ERM) family of membrane-cytoskeleton linking proteins, at a site overlapping that for AP2, a clathrin adaptor. Binding of bacterial fusion proteins confirmed this interaction. To determine whether ERM proteins interact with L1 in vivo, extracellular antibodies to L1 were used to force cluster the protein on cultured hippocampal neurons and PC12 cells, which were then immunolabeled for ERM proteins. Confocal analysis revealed a precise pattern of codistribution between ERMs and L1 clusters in axons and PC12 neurites, whereas ERMs in dendrites and spectrin labeling remained evenly distributed. Transfection of hippocampal neurons grown on an L1 substrate with a dominant negative ERM construct resulted in extensive and abnormal elaboration of membrane protrusions and an increase in axon branching, highlighting the importance of the ERM-actin interaction in axon development. Together, our data indicate that L1 binds directly to members of the ERM family and suggest this association may coordinate aspects of axonal morphogenesis.

摘要

利用轴突细胞粘附分子L1的胞质结构域筛选酵母双杂交文库,以鉴定可能参与L1功能调节的结合伙伴。L1的细胞内结构域与埃兹蛋白(ezrin)结合,埃兹蛋白是膜 - 细胞骨架连接蛋白埃兹蛋白、根蛋白和膜突蛋白(ERM)家族的成员,其结合位点与网格蛋白衔接蛋白AP2的结合位点重叠。细菌融合蛋白的结合证实了这种相互作用。为了确定ERM蛋白在体内是否与L1相互作用,使用针对L1的细胞外抗体促使该蛋白在培养的海马神经元和PC12细胞上聚集,然后对这些细胞进行ERM蛋白免疫标记。共聚焦分析显示,轴突和PC12神经突中ERM蛋白与L1簇之间存在精确的共分布模式,而树突中的ERM蛋白和血影蛋白标记仍均匀分布。用显性负性ERM构建体转染在L1底物上生长的海马神经元,导致膜突起广泛且异常地形成,轴突分支增加,突出了ERM - 肌动蛋白相互作用在轴突发育中的重要性。总之,我们的数据表明L1直接与ERM家族成员结合,并表明这种关联可能协调轴突形态发生的各个方面。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6bf4/2173555/b77c4e60b39e/0111076f1.jpg

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