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跨膜岗哨连接胞质和细胞周骨架,形成阻止受体结合的屏障。

Transmembrane Pickets Connect Cyto- and Pericellular Skeletons Forming Barriers to Receptor Engagement.

机构信息

Program in Cell Biology, Peter Gilgan Centre for Research and Learning, Hospital for Sick Children, Toronto, ON M5G 0A4, Canada.

Department of Biophysics, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.

出版信息

Cell. 2018 Jan 11;172(1-2):305-317.e10. doi: 10.1016/j.cell.2017.12.023.

Abstract

Phagocytic receptors must diffuse laterally to become activated upon clustering by multivalent targets. Receptor diffusion, however, can be obstructed by transmembrane proteins ("pickets") that are immobilized by interacting with the cortical cytoskeleton. The molecular identity of these pickets and their role in phagocytosis have not been defined. We used single-molecule tracking to study the interaction between Fcγ receptors and CD44, an abundant transmembrane protein capable of indirect association with F-actin, hence likely to serve as a picket. CD44 tethers reversibly to formin-induced actin filaments, curtailing receptor diffusion. Such linear filaments predominate in the trailing end of polarized macrophages, where receptor mobility was minimal. Conversely, receptors were most mobile at the leading edge, where Arp2/3-driven actin branching predominates. CD44 binds hyaluronan, anchoring a pericellular coat that also limits receptor displacement and obstructs access to phagocytic targets. Force must be applied to traverse the pericellular barrier, enabling receptors to engage their targets.

摘要

吞噬细胞受体必须横向扩散,才能在多价靶标聚集时被激活。然而,受体的扩散可能会被跨膜蛋白(“岗哨”)阻碍,这些蛋白通过与皮质细胞骨架相互作用而固定。这些岗哨的分子身份及其在吞噬作用中的作用尚未确定。我们使用单分子跟踪技术研究了 Fcγ 受体与 CD44 之间的相互作用,CD44 是一种丰富的跨膜蛋白,能够与 F- 肌动蛋白间接结合,因此可能作为岗哨。CD44 可逆地固定在形成素诱导的肌动蛋白丝上,限制受体的扩散。这种线性丝在极化巨噬细胞的尾部占主导地位,受体的流动性最小。相反,受体在前沿的流动性最大,那里 Arp2/3 驱动的肌动蛋白分支占主导地位。CD44 结合透明质酸,锚定细胞周围的外壳,也限制受体位移并阻碍吞噬靶标的进入。必须施加力才能穿过细胞周围的屏障,使受体能够与其靶标结合。

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