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Nucleus downscaling in mouse embryos is regulated by cooperative developmental and geometric programs

机译:小鼠胚胎中的细胞核缩小受协同发展和几何程序的调节

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摘要

Maintaining appropriate nucleus size is important for cell health, but the mechanisms by which this is achieved are poorly understood. Controlling nucleus size is a particular challenge in early development, where the nucleus must downscale in size with progressive reductive cell divisions. Here we use live and fixed imaging, micromanipulation approaches, and small molecule analyses during preimplantation mouse development to probe the mechanisms by which nucleus size is determined. We find a close correlation between cell and nuclear size at any given developmental stage, and show that experimental cytoplasmic reduction can alter nuclear size, together indicating that cell size helps dictate nuclear proportions. Additionally, however, by creating embryos with over-sized blastomeres we present evidence of a developmental program that drives nuclear downscaling independently of cell size. We show that this developmental program does not correspond with nuclear import rates, but provide evidence that PKC activity may contribute to this mechanism. We propose a model in which nuclear size regulation during early development is a multi-mode process wherein nucleus size is set by cytoplasmic factors, and fine-tuned on a cell-by-cell basis according to cell size.
机译:维持适当的细胞核大小对于细胞健康很重要,但是实现该机制的机制却鲜为人知。在早期发育中,控制细胞核的大小是一个特殊的挑战,在该过程中,细胞核的大小必须随着渐进的还原性细胞分裂而缩小。在这里,我们在植入前小鼠发育过程中使用实时和固定成像,显微操作方法以及小分子分析来探查确定核大小的机制。我们发现在任何给定的发育阶段细胞与核大小之间都具有密切的相关性,并表明实验性细胞质的减少可以改变核大小,共同表明细胞大小有助于决定核的比例。但是,此外,通过创建带有超大卵裂球的胚胎,我们提供了一个发育程序的证据,该程序可以独立于细胞大小而驱动核的缩小。我们表明,这一发展计划与核进口率不符,但提供了证明PKC活动可能有助于这种机制的证据。我们提出了一个模型,其中早期发育过程中的核大小调节是一个多模式过程,其中核大小由细胞质因子设定,并根据细胞大小在逐个细胞的基础上进行微调。

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