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Dynamics of transitional endoplasmic reticulum sites in vertebrate cells

机译:脊椎动物细胞中过渡型内质网位点的动力学

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摘要

A typical vertebrate cell contains several hundred sites of transitional ER (tER). Presumably, tER sites generate elements of the ER-Golgi intermediate compartment (ERGIC), and ERGIC elements then generate Golgi cisternae. Therefore, characterizing the mechanisms that influence tER distribution may shed light on the dynamic behavior of the Golgi. We explored the properties of tER sites using Sec13 as a marker protein. Fluorescence microscopy confirmed that tER sites are long-lived ER subdomains. tER sites proliferate during interphase but lose Sec13 during mitosis. Unlike ERGIC elements, tER sites move very little. Nevertheless, when microtubules are depolymerized with nocodazole, tER sites redistribute rapidly to form clusters next to Golgi structures. Hence, tER sites have the unusual property of being immobile, yet dynamic. These findings can be explained by a model in which new tER sites are created by retrograde membrane traffic from the Golgi. We propose that the tER-Golgi system is organized by mutual feedback between these two compartments. [References: 98]
机译:典型的脊椎动物细胞包含数百个过渡型ER(tER)。据推测,tER位点产生了ER-高尔基体中间区室(ERGIC)的元素,而ERGIC元素则产生了高尔基池。因此,表征影响tER分布的机制可能会阐明高尔基体的动态行为。我们探索了使用Sec13作为标记蛋白的tER位点的属性。荧光显微镜证实,tER位点是长寿命的ER亚结构域。 tER位点在相间期增生,但在有丝分裂期丢失Sec13。与ERGIC元素不同,tER站点移动很少。然而,当微管与诺考达唑解聚时,tER位点迅速重新分布,形成高尔基体旁边的簇。因此,tER站点具有不移动但动态的非凡特性。这些发现可以通过一个模型来解释,在该模型中,来自高尔基体的逆行膜运输产生了新的tER位点。我们建议通过这两个区室之间的相互反馈来组织tER-Golgi系统。 [参考:98]

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