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多样化的肌动蛋白突起促进了环境探索,但对于白细胞的运动却是可有可无的。

Diversified actin protrusions promote environmental exploration but are dispensable for locomotion of leukocytes.

机构信息

Institute of Science and Technology Austria (IST Austria), am Campus 1, 3400 Klosterneuburg, Austria.

Institute for Molecular Biotechnology, Austrian Academy of Sciences, Dr. Bohr-Gasse 3, 1030 Vienna, Austria.

出版信息

Nat Cell Biol. 2016 Nov;18(11):1253-1259. doi: 10.1038/ncb3426. Epub 2016 Oct 24.

Abstract

Most migrating cells extrude their front by the force of actin polymerization. Polymerization requires an initial nucleation step, which is mediated by factors establishing either parallel filaments in the case of filopodia or branched filaments that form the branched lamellipodial network. Branches are considered essential for regular cell motility and are initiated by the Arp2/3 complex, which in turn is activated by nucleation-promoting factors of the WASP and WAVE families. Here we employed rapid amoeboid crawling leukocytes and found that deletion of the WAVE complex eliminated actin branching and thus lamellipodia formation. The cells were left with parallel filaments at the leading edge, which translated, depending on the differentiation status of the cell, into a unipolar pointed cell shape or cells with multiple filopodia. Remarkably, unipolar cells migrated with increased speed and enormous directional persistence, while they were unable to turn towards chemotactic gradients. Cells with multiple filopodia retained chemotactic activity but their migration was progressively impaired with increasing geometrical complexity of the extracellular environment. These findings establish that diversified leading edge protrusions serve as explorative structures while they slow down actual locomotion.

摘要

大多数迁移细胞通过肌动蛋白聚合的力将其前缘挤出。聚合需要一个初始成核步骤,该步骤由在丝状伪足的情况下建立平行丝或形成分支片状伪足网络的分支丝的因子来介导。分支被认为是正常细胞运动所必需的,并且由 Arp2/3 复合物引发,该复合物反过来又被 WAVE 家族的成核促进因子激活。在这里,我们使用快速变形虫样游走的白细胞,并发现 WAVE 复合物的缺失消除了肌动蛋白的分支,从而也消除了片状伪足的形成。细胞在前沿留下平行丝,这取决于细胞的分化状态,转化为单极尖形细胞形状或具有多个丝状伪足的细胞。值得注意的是,单极细胞以增加的速度和巨大的方向持久性迁移,而它们无法转向趋化性梯度。具有多个丝状伪足的细胞保留趋化性活性,但随着细胞外环境几何复杂性的增加,它们的迁移逐渐受到损害。这些发现表明,多样化的前沿突起作为探索性结构,同时减缓了实际的运动。

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