Institut Pasteur, Unité des Interactions Bactéries-Cellules, Paris, F-75015, France.
Traffic. 2012 Dec;13(12):1653-66. doi: 10.1111/tra.12009. Epub 2012 Oct 11.
Invasive bacterial pathogens often target cellular proteins involved in adhesion as a first event during infection. For example, Listeria monocytogenes uses the bacterial protein InlA to interact with E-cadherin, hijack the host adherens junction (AJ) machinery and invade non-phagocytic cells by a clathrin-dependent mechanism. Here, we investigate a potential role for clathrin in cell-cell adhesion. We observed that the initial steps of AJ formation trigger the phosphorylation of clathrin, and its transient localization at forming cell-cell contacts. Furthermore, we show that clathrin serves as a hub for the recruitment of proteins that are necessary for the actin rearrangements that accompany the maturation of AJs. Using an InlA/E-cadherin chimera, we show that adherent cells expressing the chimera form AJs with cells expressing E-cadherin. We demonstrate that non-adherent cells expressing the InlA chimera, as bacteria, can be internalized by E-cadherin-expressing adherent cells. Together these results reveal that a common clathrin-mediated machinery may regulate internalization and cell adhesion and that the relative mobility of one of the interacting partners plays an important role in the commitment to either one of these processes.
侵袭性细菌病原体通常将细胞内参与黏附的蛋白质作为感染过程中的第一个目标。例如,李斯特菌(Listeria monocytogenes)利用细菌蛋白 InlA 与上皮钙黏蛋白(E-cadherin)相互作用,劫持宿主黏着连接(adherens junction,AJ)机制,并通过网格蛋白依赖的机制侵入非吞噬细胞。在这里,我们研究了网格蛋白在细胞-细胞黏附中的潜在作用。我们观察到 AJ 形成的初始步骤会触发网格蛋白的磷酸化,并使其短暂定位于形成的细胞-细胞接触处。此外,我们表明网格蛋白作为募集参与伴随 AJ 成熟的肌动蛋白重排的蛋白质的枢纽。使用 InlA/E-cadherin 嵌合体,我们表明表达嵌合体的黏附细胞与表达 E-cadherin 的细胞形成 AJ。我们证明,表达 InlA 嵌合体的非黏附细胞(如同细菌)可以被表达 E-cadherin 的黏附细胞内化。这些结果表明,一种常见的网格蛋白介导的机制可能调节内化和细胞黏附,并且相互作用的一个伴侣的相对迁移性在决定这两个过程中的任何一个过程中起着重要作用。
