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高尔基体在完全组装之前进行货物运输的能力。

Capacity of the Golgi apparatus for cargo transport prior to complete assembly.

作者信息

Jiang Shu, Rhee Sung W, Gleeson Paul A, Storrie Brian

机构信息

Department of Physiology and Biophysics, University of Arkansas for Medical Sciences, Little Rock, AR 72205, USA.

出版信息

Mol Biol Cell. 2006 Sep;17(9):4105-17. doi: 10.1091/mbc.e05-12-1112. Epub 2006 Jul 12.

Abstract

In yeast, particular emphasis has been given to endoplasmic reticulum (ER)-derived, cisternal maturation models of Golgi assembly while in mammalian cells more emphasis has been given to golgins as a potentially stable assembly framework. In the case of de novo Golgi formation from the ER after brefeldin A/H89 washout in HeLa cells, we found that scattered, golgin-enriched, structures formed early and contained golgins including giantin, ranging across the entire cis to trans spectrum of the Golgi apparatus. These structures were incompetent in VSV-G cargo transport. Second, we compared Golgi competence in cargo transport to the kinetics of addition of various glycosyltransferases and glycosidases into nascent, golgin-enriched structures after drug washout. Enzyme accumulation was sequential with trans and then medial glycosyltransferases/glycosidases found in the scattered, nascent Golgi. Involvement in cargo transport preceded full accumulation of enzymes or GPP130 into nascent Golgi. Third, during mitosis, we found that the formation of a golgin-positive acceptor compartment in early telophase preceded the accumulation of a Golgi glycosyltransferase in nascent Golgi structures. We conclude that during mammalian Golgi assembly components fit into a dynamic, first-formed, multigolgin-enriched framework that is initially cargo transport incompetent. Resumption of cargo transport precedes full Golgi assembly.

摘要

在酵母中,人们特别强调了内质网(ER)衍生的高尔基体组装的扁平囊成熟模型,而在哺乳动物细胞中,人们更强调高尔基体蛋白作为一个潜在的稳定组装框架。在HeLa细胞中用布雷菲德菌素A/H89洗脱后从内质网重新形成高尔基体的情况下,我们发现,早期形成了分散的、富含高尔基体蛋白的结构,其中包含高尔基体蛋白,包括巨蛋白,横跨高尔基体从顺面到反面的整个区域。这些结构在VSV-G货物运输方面无功能。其次,我们将货物运输中的高尔基体功能与药物洗脱后各种糖基转移酶和糖苷酶添加到新生的、富含高尔基体蛋白的结构中的动力学进行了比较。酶的积累是顺序性的,在分散的新生高尔基体中先发现反面糖基转移酶/糖苷酶,然后是中间糖基转移酶/糖苷酶。参与货物运输先于酶或GPP130完全积累到新生高尔基体中。第三,在有丝分裂期间,我们发现末期早期高尔基体蛋白阳性受体区室的形成先于高尔基体糖基转移酶在新生高尔基体结构中的积累。我们得出结论,在哺乳动物高尔基体组装过程中,各组分融入一个动态的、首先形成的、富含多种高尔基体蛋白的框架,该框架最初无货物运输功能。货物运输的恢复先于完整的高尔基体组装。

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