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EB1 and cytoplasmic dynein mediate protrusion dynamics for efficient 3-dimensional cell migration

机译:EB1和细胞质动力蛋白介导突起动力学以实现有效的3维细胞迁移

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摘要

Microtubules have long been implicated to play an integral role in metastatic disease, for which a critical step is the local invasion of tumor cells into the 3-dimensional (3D) collagen-rich stromal matrix. Here we show that cell migration of human cancer cells uses the dynamic formation of highly branched protrusions that are composed of a microtubule core surrounded by cortical actin, a cytoskeletal organization that is absent in cells on 2-dimensional (2D) substrates. Microtubule plus-end tracking protein End-binding 1 and motor protein dynein subunits light intermediate chain 2 and heavy chain 1, which do not regulate 2D migration, critically modulate 3D migration by affecting RhoA and thus regulate protrusion branching through differential assembly dynamics of microtubules. An important consequence of this observation is that the commonly used cancer drug paclitaxel is 100-fold more effective at blocking migration in a 3D matrix than on a 2D matrix. This work reveals the central role that microtubule dynamics plays in powering cell migration in a more pathologically relevant setting and suggests further testing of therapeutics targeting microtubules to mitigate migration.—Jayatilaka, H., Giri, A., Karl, M., Aifuwa, I., Trenton, N. J., Phillip, J. M., Khatau, S., Wirtz, D. EB1 and cytoplasmic dynein mediate protrusion dynamics for efficient 3-dimensional cell migration.
机译:长期以来,人们一直认为微管在转移性疾病中起着不可或缺的作用,其关键步骤是肿瘤细胞局部侵入富含3维(3D)胶原蛋白的基质中。在这里,我们显示人类癌细胞的细胞迁移利用了高度分支的突起的动态形成,该突起由被皮质肌动蛋白包围的微管核心组成,皮质肌动蛋白是二维(2D)基质上的细胞中不存在的细胞骨架组织。微管正端跟踪蛋白末端结合1和运动蛋白达因蛋白亚基轻中链2和重链1,它们不调节2D迁移,而是通过影响RhoA来关键地调节3D迁移,从而通过微管的不同组装动力学来调节突起分支。该观察结果的重要结果是,常用的癌症药物紫杉醇在3D基质中阻止迁移的作用比在2D基质上有效100倍。这项工作揭示了微管动力学在更病理相关的环境中在促进细胞迁移中发挥的核心作用,并建议针对微管以减轻迁移的治疗药物进行进一步测试。—Jayatilaka,H.,Giri,A.,Karl,M.,Aifuwa, I.,Trenton,NJ,Phillip,JM,Khatau,S.,Wirtz,D.EB1和细胞质动力蛋白为有效的3维细胞迁移介导突出动力学。

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