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Regulation of ECM degradation and axon guidance by growth cone invadosomes

机译:生长锥侵染小体对ECM降解和轴突引导的调节

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Invadopodia and podosomes, collectively referred to as invadosomes, are F-actin-rich basal protrusions of cells that provide sites of attachment to and degradation of the extracellular matrix. Invadosomes promote the invasion of cells, ranging from metastatic cancer cells to immune cells, into tissue. Here, we show that neuronal growth cones form protrusions that share molecular, structural and functional characteristics of invadosomes. Growth cones from all neuron types and species examined, including a variety of human neurons, form invadosomes both in vitro and in vivo. Growth cone invadosomes contain dynamic F-actin and several actin regulatory proteins, as well as Tks5 and matrix metalloproteinases, which locally degrade the matrix. When viewed using three-dimensional super-resolution microscopy, F-actin foci often extended together with microtubules within orthogonal protrusions emanating from the growth cone central domain. Finally, inhibiting the function of Tks5 both reduced matrix degradation in vitro and disrupted motoneuron axons from exiting the spinal cord and extending into the periphery. Taken together, our results suggest that growth cones use invadosomes to target protease activity during axon guidance through tissues.
机译:侵染足和足小体,统称为侵染小体,是细胞富含F-肌动蛋白的基础突起,提供与细胞外基质的附着和降解位点。侵染体促进从转移性癌细胞到免疫细胞的细胞向组织的侵袭。在这里,我们显示神经元生长锥形成了突起,这些突起共享入侵小体的分子,结构和功能特征。来自所检查的所有神经元类型和物种的生长锥,包括各种人类神经元,在体外和体内均形成侵染体。生长锥invadosomes包含动态的F-肌动蛋白和一些肌动蛋白调节蛋白,以及Tks5和基质金属蛋白酶,它们会局部降解基质。当使用三维超高分辨率显微镜观察时,F-肌动蛋白病灶通常与微管一起在生长锥中央区域发出的正交突起内延伸。最后,抑制Tks5的功能既减少了体外基质降解,又破坏了运动神经元轴突离开脊髓并延伸到周围。两者合计,我们的结果表明,生长锥使用轴突引导通过组织的轴突过程中的蛋白酶体。

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