Nucleating amoeboid cancer cell motility with Diaphanous related formins.

Neelakshi Kar, Jeremy S Logue
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Abstract

The tissue invasive capacity of cancer cells is determined by their phenotypic plasticity. For instance, mesenchymal to amoeboid transition has been found to facilitate the passage of cancer cells through confined environments. This phenotypic transition is also heavily regulated by the architecture of the actin cytoskeleton, which may increase myosin contractility and the intracellular pressure that is known to drive bleb formation. In this review, we highlight several Diaphanous related formins (DRFs) that have been found to promote or suppress bleb formation in cancer cells, which is a hallmark of amoeboid migration. Based on the work discussed here, the role of the DRFs in cancer(s) is worthy of further scrutiny in animal models, as they may prove to be therapeutic targets.

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用与Diaphanous相关的甲形蛋白核化变形虫癌细胞的运动性。
癌细胞的表型可塑性决定了其组织侵袭能力。例如,研究发现,间质细胞向变形细胞的转变有助于癌细胞通过封闭的环境。这种表型转变还在很大程度上受肌动蛋白细胞骨架结构的调控,肌动蛋白细胞骨架结构可能会增加肌动蛋白的收缩能力和细胞内压力,而细胞内压力是已知的瘤疱形成的驱动力。在这篇综述中,我们重点介绍了几种已被发现能促进或抑制癌细胞蚕泡形成的Diaphanous related formins (DRFs),蚕泡形成是变形虫迁移的一个标志。根据本文讨论的工作,DRFs 在癌症中的作用值得在动物模型中进一步研究,因为它们可能被证明是治疗靶点。
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