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Cell Adh Migr


Cell Adh Migr
影响因子: 2.336
I S S N: 1933-6918
出 版 社: Landes Bioscience
出 版 地: Austin, Tex.
出版国家: United States
刊  期: 季刊
创刊时间: 2007
语  种: 英文
审稿周期: 较慢,6-12周
中科院分区:
投稿命中率: 较易
国外数据库收录: IM
中国收录文章数: 1
5年影响因子: 2.298
研究领域: 细胞粘附、细胞运动
官方链接: https://www.landesbioscience.com/journals/celladhe...
投稿须知: https://www.landesbioscience.com/journals/celladhe...

期刊介绍:

Cell-cell adhesion is a critical process for the formation and maintenance of tissue patterns during development, as well as invasion and metastasis of cancer cells. Although great strides have been made regarding our understanding of the processes that play a role in cell-cell adhesion, the precise mechanisms by which diverse signaling events regulate cell and tissue architecture is poorly understood.  In a recent study using the epithelial cells of early stage Xenopus embryos, we have shown that loss- or gain-of function of ephrinB1 can disrupt cell-cell contacts and tight junctions. This study reveals a mechanism where ephrinB1 competes with active Cdc42 for binding to Par-6, a scaffold protein central to the Par polarity complex (Par-3/Par-6/Cdc42/aPKC) and disrupts the localization of tight junction-associated proteins (ZO-1, Cingulin) at tight junctions. This competition reduces aPKC activity critical to maintaining and/or forming tight junctions. Finally, phosphorylation of ephrinB1 on specific tyrosine residues can block the interaction between ephrinB1 and Par-6 at tight junctions, and restore tight junction formation. Recent evidence indicates that de-regulation of forward signaling through EphB receptors may play a role in metastatic progression in colon cancer. In light of the new data showing an effect of ephrinB reverse signaling on tight junctions, an additional mechanism can be hypothesized where de-regulation of ephrinB1 expression or phosphorylation may also impact metastatic progression.
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