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首页> 外文期刊>Nature Communications >The post-abscission midbody is an intracellular signaling organelle that regulates cell proliferation
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The post-abscission midbody is an intracellular signaling organelle that regulates cell proliferation

机译:脱落后嗜含量是调节细胞增殖的细胞内信号细胞器

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摘要

Once thought to be a remnant of cell division, the midbody (MB) has recently been shown to have roles beyond its primary function of orchestrating abscission. Despite the emerging roles of post-abscission MBs, how MBs accumulate in the cytoplasm and signal to regulate cellular functions remains unknown. Here, we show that extracellular post-abscission MBs can be internalized by interphase cells, where they reside in the cytoplasm as a membrane-bound signaling structure that we have named the MBsome. We demonstrate that MBsomes stimulate cell proliferation and that MBsome formation is a phagocytosis-like process that depends on a phosphatidylserine/integrin complex, driven by actin-rich membrane protrusions. Finally, we show that MBsomes rely on dynamic actin coats to slow lysosomal degradation and propagate their signaling function. In summary, MBsomes may sometimes serve as intracellular organelles that signal via integrin and EGFR-dependent pathways to promote cell proliferation and anchorage-independent growth and survival.
机译:一旦被认为是细胞分裂的残余,最近被证明了中间(MB)具有超出其协调脱落的主要功能的作用。尽管脱落后MBS的新兴作用,但MBS如何在细胞质中积聚,以调节细胞功能仍然未知。在这里,我们表明细胞外脱落MBS可以通过间间细胞内化,其中它们在细胞质中作为膜结合的信令结构,我们已经命名为MBSome。我们证明了MBSOMES刺激细胞增殖,并且MBSome形成是一种吞噬症状的方法,其取决于由富含致动蛋白的膜突起驱动的磷脂酰丝氨酸/整联蛋白复合物。最后,我们表明,MBSomes依赖于动态肌动蛋白涂层以缓慢溶酶体降解并传播它们的信号功能。总之,MBSOMES有时可以用作通过整联蛋白和EGFR依赖性途径发出的细胞内细胞器,以促进细胞增殖和锚定无关的生长和存活。

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