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      PDMP Blocks Brefeldin A–induced Retrograde Membrane Transport from Golgi to ER: Evidence for Involvement of Calcium Homeostasis and Dissociation from Sphingolipid Metabolism

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          Abstract

          In this study, we show that an inhibitor of sphingolipid biosynthesis, d, l- threo-1-phenyl-2- decanoylamino-3-morpholino-1-propanol (PDMP), inhibits brefeldin A (BFA)-induced retrograde membrane transport from Golgi to endoplasmic reticulum (ER). If BFA treatment was combined with or preceded by PDMP administration to cells, disappearance of discrete Golgi structures did not occur. However, when BFA was allowed to exert its effect before PDMP addition, PDMP could not “rescue” the Golgi compartment.

          Evidence is presented showing that this action of PDMP is indirect, which means that the direct target is not sphingolipid metabolism at the Golgi apparatus. A fluorescent analogue of PDMP, 6-( N-[7-nitro-2,1,3-benzoxadiazol-4-yl]amino)hexanoyl-PDMP (C 6-NBD-PDMP), did not localize in the Golgi apparatus. Moreover, the effect of PDMP on membrane flow did not correlate with impaired C 6-NBD-sphingomyelin biosynthesis and was not mimicked by exogenous C 6-ceramide addition or counteracted by exogenous C 6-glucosylceramide addition. On the other hand, the PDMP effect was mimicked by the multidrug resistance protein inhibitor MK571.

          The effect of PDMP on membrane transport correlated with modulation of calcium homeostasis, which occurred in a similar concentration range. PDMP released calcium from at least two independent calcium stores and blocked calcium influx induced by either extracellular ATP or thapsigargin. Thus, the biological effects of PDMP revealed a relation between three important physiological processes of multidrug resistance, calcium homeostasis, and membrane flow in the ER/ Golgi system.

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          A rapid method of total lipid extraction and purification.

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            Rapid redistribution of Golgi proteins into the ER in cells treated with brefeldin A: Evidence for membrane cycling from Golgi to ER

            In cells treated with brefeldin A (BFA), movement of newly synthesized membrane proteins from the endoplasmic reticulum (ER) to the Golgi apparatus was blocked. Surprisingly, the glycoproteins retained in the ER were rapidly processed by cis/medial Golgi enzymes but not by trans Golgi enzymes. An explanation for these observations was provided from morphological studies at both the light and electron microscopic levels using markers for the cis/medial and trans Golgi. They revealed a rapid and dramatic redistribution to the ER of components of the cis/medial but not the trans Golgi in response to treatment with BFA. Upon removal of BFA, the morphology of the Golgi apparatus was rapidly reestablished and proteins normally transported out of the ER were efficiently and rapidly sorted to their final destinations. These results suggest that BFA disrupts a dynamic membrane-recycling pathway between the ER and cis/medial Golgi, effectively blocking membrane transport out of but not back to the ER.
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              Brefeldin A: insights into the control of membrane traffic and organelle structure

              (1992)
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                Author and article information

                Journal
                J Cell Biol
                The Journal of Cell Biology
                The Rockefeller University Press
                0021-9525
                1540-8140
                13 July 1998
                : 142
                : 1
                : 25-38
                Affiliations
                [* ]Department of Physiological Chemistry, []Department of Clinical Pharmacology, University of Groningen, Groningen Institute for Drug Studies (GIDS), 9713 AV Groningen, The Netherlands; and [§ ]Universitat de Barcelona, Facultat de Medicina, Departament de Biologia Cellular, Institut d'Investigacions Biomediques August Pi I Sunyer, 08036 Barcelona, Spain
                Article
                10.1083/jcb.142.1.25
                2133041
                9660860
                ac8ac2c1-d304-4461-9dc2-2f4b8f907697
                Copyright @ 1998
                History
                : 9 December 1997
                : 27 May 1998
                Categories
                Articles

                Cell biology
                ceramide,retrograde membrane flow,β-cop,multidrug resistance,intracellular calcium
                Cell biology
                ceramide, retrograde membrane flow, β-cop, multidrug resistance, intracellular calcium

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