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Structural determinants of Junctional Adhesion Molecule A (JAM-A) function and mechanisms of intracellular signaling

机译:结缔合分子A(JAM-A)功能的结构决定因素和细胞内信号传导的机制

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摘要

Junctional Adhesion Molecule A (JAM-A) is a multifunctional cell surface protein that has multiple evolutionarily conserved structural features. There is now conclusive evidence that discrete structural elements on JAM-A mediate intracellular signaling events that alter cell migration and paracellular permeability. Specifically, self-dimerization between extracellular Ig-like loops and close apposition of PDZ-dependent, JAM-A-associated intracellular scaffold proteins such as Afadin and guanine-nucleotide exchange factors mediate activation of Rap1 and modulation of epithelial cell migration by effects on beta1 integrin. While the same JAM-A structural features also modulate migration of other cell types and paracellular permeability in epithelia/endothelia, additional signaling proteins/mechanisms are probably involved. Recent insights into JAM-A outside-in signaling events that regulate these cellular functions are discussed.
机译:结黏附分子A(JAM-A)是一种多功能的细胞表面蛋白,具有多种进化保守的结构特征。现在有确凿的证据表明,JAM-A上的离散结构元件介导了改变细胞迁移和细胞旁通透性的细胞内信号传导事件。具体来说,细胞外Ig样环之间的自我二聚化和PDZ依赖的,与JAM-A相关的细胞内支架蛋白(如Afadin和鸟嘌呤核苷酸交换因子)的紧密并置介导Rap1的激活和对beta1的影响对上皮细胞迁移的调节。整合素尽管相同的JAM-A结构特征还可以调节其他细胞类型的迁移和上皮/内皮细胞的细胞旁通透性,但可能还涉及其他信号蛋白/机制。讨论了对调节这些细胞功能的JAM-A由内而外的信号事件的最新见解。

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