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Golgi Inheritance Under a Block of Anterograde and Retrograde Traffic
Author(s) -
Nizak Clément,
Sougrat Rachid,
Jollivet Florence,
Rambourg Alain,
Goud Bruno,
Perez Franck
Publication year - 2004
Publication title -
traffic
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.677
H-Index - 130
eISSN - 1600-0854
pISSN - 1398-9219
DOI - 10.1111/j.1398-9219.2004.0174.x
Subject(s) - golgi apparatus , mitosis , cell plate , microbiology and biotechnology , brefeldin a , endoplasmic reticulum , biology , prometaphase , organelle , metaphase , secretory pathway , microtubule , cell , cell division , genetics , cytokinesis , chromosome , gene
In mitosis, the Golgi complex is inherited following its dispersion, equal partitioning and reformation in each daughter cell. The state of Golgi membranes during mitosis is controversial, and the role of Golgi‐intersecting traffic in Golgi inheritance is unclear. We have used brefeldin A (BFA) to perturb Golgi‐intersecting membrane traffic at different stages of the cell cycle and followed by live cell imaging the fate of Golgi membranes in those conditions. We observed that addition of the drug on cells in prometaphase prevents mitotic Golgi dispersion. Under continuous treatment, Golgi fragments persist throughout mitosis and accumulate in a Golgi‐like structure at the end of mitosis. This structure localizes at microtubule minus ends and contains all classes of Golgi markers, but is not accessible to cargo from the endoplasmic reticulum or the plasma membrane because of the continuous BFA traffic block. However, it contains preaccumulated cargo, and intermixes with the reforming Golgi upon BFA washout. This structure also forms when BFA is added during metaphase, when the Golgi is not discernible by light microscopy. Together the data indicate that independent Golgi fragments that contain all classes of Golgi markers (and that can be isolated from other organelles by blocking anterograde and retrograde Golgi‐intersecting traffic) persist throughout mitosis.

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