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Dynamics and organization of the transitional endoplasmic reticulum and the Golgi apparatus.

机译:动态和组织的过渡内质网和高尔基体。

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摘要

The Golgi apparatus performs central functions in the secretory pathway by processing and sorting secretory material and synthesizing certain lipids. These biochemical events are well characterized, but the mechanism by which secretory cargo flows through the Golgi is an area of intense debate. A popular model for Golgi organization is the maturation model, which proposes that Golgi cisternae are transient structures that progress through the stack, maturing in the process, until they ultimately break up into secretory and transport vesicles. In the maturation model, new Golgi cisternae are produced by the coalescence of ER-derived COPII vesicles. These vesicles bud from specialized subdomains of the ER called transitional ER (tER) sites. Thus, the tER represents the birthplace of the Golgi. To gain a better understanding of the Golgi, we need to determine the nature of the tER. The tER has not been well characterized in the past due to the technical difficulty of visualizing this compartment. I overcame this hurdle by developing two methods for examining the tER that have allowed me to greatly extend our understanding. First, I devised an improved immunofluorescence protocol that yields superb preservation of tER sites and other small cellular structures. Using this protocol, I was able to observe the organization of the tER in mammalian cells under a variety of conditions. I also used this protocol to quantify the relationship between tER activity and Golgi disassembly during mammalian mitosis. Second, I developed a system for accelerating the acquisition of 4D image sets of living cells. This Fast-4D system, in combination with a GFP-tagged tER marker allowed for a detailed analysis of tER sites in the yeast Pichia pastoris. From these experiments we concluded that the tER is an independent long-lived ER subdomain that is not directly positioned by the cytoskeleton. Our video data show that tER sites can form de novo and are capable of fusing with one another but do not appear to divide. These observations have led to a model that explains the organization and propagation of tER sites.
机译:高尔基体通过处理和分类分泌物质并合成某些脂质来在分泌途径中发挥重要作用。这些生化事件具有很好的特征,但是分泌性货物流过高尔基体的机制是一个激烈争论的领域。成熟模型是高尔基组织的一种流行模型,该模型提出高尔基池是过渡的结构,在整个过程中逐渐成熟,直到最终分解为分泌和运输的囊泡。在成熟模型中,通过ER衍生的COPII囊泡的聚结产生了新的高尔基水箱。这些囊泡从称为过渡性ER(tER)位点的ER的专门亚域中萌芽。因此,tER代表高尔基的发源地。为了更好地了解高尔基体,我们需要确定tER的性质。由于可视化该隔室的技术难度,tER过去没有得到很好的表征。通过开发两种检查tER的方法,我克服了这一障碍,这使我大大扩展了我们的理解。首先,我设计了一种改进的免疫荧光方案,可以很好地保存tER位点和其他小细胞结构。使用此协议,我能够在多种条件下观察哺乳动物细胞中tER的组织。我还使用此协议来量化哺乳动物有丝分裂期间tER活性与高尔基体拆卸之间的关系。其次,我开发了一种用于加速采集活细胞4D图像集的系统。这种Fast-4D系统与GFP标记的tER标记结合使用,可以对酵母毕赤酵母中的tER位点进行详细分析。从这些实验中,我们得出结论,tER是一个独立的长寿命ER子域,不会直接被细胞骨架定位。我们的视频数据显示,tER位点可以从头形成,并且可以相互融合,但似乎不会分裂。这些观察结果导致建立了一个模型,解释了tER位点的组织和传播。

著录项

  • 作者

    Hammond, Adam Thomas.;

  • 作者单位

    The University of Chicago.;

  • 授予单位 The University of Chicago.;
  • 学科 Biology Cell.
  • 学位 Ph.D.
  • 年度 2001
  • 页码 143 p.
  • 总页数 143
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 宗教;
  • 关键词

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