Literature DB >> 20947505

Heteromeric interactions required for abundance and subcellular localization of human CDC50 proteins and class 1 P4-ATPases.

Lieke M van der Velden1, Catharina G K Wichers, Adriana E D van Breevoort, Jonathan A Coleman, Robert S Molday, Ruud Berger, Leo W J Klomp, Stan F J van de Graaf.   

Abstract

Members of the P(4) family of P-type ATPases (P(4)-ATPases) are believed to function as phospholipid flippases in complex with CDC50 proteins. Mutations in the human class 1 P(4)-ATPase gene ATP8B1 cause a severe syndrome characterized by impaired bile flow (intrahepatic cholestasis), often leading to end-stage liver failure in childhood. In this study, we determined the specificity of human class 1 P(4)-ATPase interactions with CDC50 proteins and the functional consequences of these interactions on protein abundance and localization of both protein classes. ATP8B1 and ATP8B2 co-immunoprecipitated with CDC50A and CDC50B, whereas ATP8B4, ATP8A1, and ATP8A2 associated only with CDC50A. ATP8B1 shifted from the endoplasmic reticulum (ER) to the plasma membrane upon coexpression of CDC50A or CDC50B. ATP8A1 and ATP8A2 translocated from the ER to the Golgi complex and plasma membrane upon coexpression of CDC50A, but not CDC50B. ATP8B2 and ATP8B4 already displayed partial plasma membrane localization in the absence of CDC50 coexpression but displayed a large increase in plasma membrane abundance upon coexpression of CDC50A. ATP8B3 did not bind CDC50A and CDC50B and was invariably present in the ER. Our data show that interactions between CDC50 proteins and class 1 P(4)-ATPases are essential for ER exit and stability of both subunits. Furthermore, the subcellular localization of the complex is determined by the P(4)-ATPase, not the CDC50 protein. The interactions of CDC50A and CDC50B with multiple members of the human P(4)-ATPase family suggest that these proteins perform broader functions in human physiology than thus far assumed.

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Year:  2010        PMID: 20947505      PMCID: PMC3000991          DOI: 10.1074/jbc.M110.139006

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  38 in total

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3.  Drs2p-dependent formation of exocytic clathrin-coated vesicles in vivo.

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Journal:  Curr Biol       Date:  2002-09-17       Impact factor: 10.834

4.  The cloning and characterization of the CDC50 gene family in Saccharomyces cerevisiae.

Authors:  M Radji; J M Kim; T Togan; H Yoshikawa; K Shirahige
Journal:  Yeast       Date:  2001-02       Impact factor: 3.239

5.  A flippase-independent function of ATP8B1, the protein affected in familial intrahepatic cholestasis type 1, is required for apical protein expression and microvillus formation in polarized epithelial cells.

Authors:  Patricia M Verhulst; Lieke M van der Velden; Viola Oorschot; Ernst E van Faassen; Judith Klumperman; Roderick H J Houwen; Thomas G Pomorski; Joost C M Holthuis; Leo W J Klomp
Journal:  Hepatology       Date:  2010-06       Impact factor: 17.425

6.  A novel membrane protein, Ros3p, is required for phospholipid translocation across the plasma membrane in Saccharomyces cerevisiae.

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Journal:  J Biol Chem       Date:  2002-07-19       Impact factor: 5.157

7.  Cdc50p, a protein required for polarized growth, associates with the Drs2p P-type ATPase implicated in phospholipid translocation in Saccharomyces cerevisiae.

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Journal:  Mol Biol Cell       Date:  2004-04-16       Impact factor: 4.138

8.  Progressive familial intrahepatic cholestasis type 1 and extrahepatic features: no catch-up of stature growth, exacerbation of diarrhea, and appearance of liver steatosis after liver transplantation.

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Authors:  Thomas Pomorski; Ruben Lombardi; Howard Riezman; Philippe F Devaux; Gerrit van Meer; Joost C M Holthuis
Journal:  Mol Biol Cell       Date:  2003-03       Impact factor: 4.138

10.  Role for Drs2p, a P-type ATPase and potential aminophospholipid translocase, in yeast late Golgi function.

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Journal:  J Cell Biol       Date:  1999-12-13       Impact factor: 10.539

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  50 in total

1.  Critical role of a transmembrane lysine in aminophospholipid transport by mammalian photoreceptor P4-ATPase ATP8A2.

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2.  Human TMEM30a promotes uptake of antitumor and bioactive choline phospholipids into mammalian cells.

Authors:  Rui Chen; Erin Brady; Thomas M McIntyre
Journal:  J Immunol       Date:  2011-02-02       Impact factor: 5.422

3.  Yeast and human P4-ATPases transport glycosphingolipids using conserved structural motifs.

Authors:  Bartholomew P Roland; Tomoki Naito; Jordan T Best; Cayetana Arnaiz-Yépez; Hiroyuki Takatsu; Roger J Yu; Hye-Won Shin; Todd R Graham
Journal:  J Biol Chem       Date:  2018-12-10       Impact factor: 5.157

4.  Phospholipid Flippase ATP10A Translocates Phosphatidylcholine and Is Involved in Plasma Membrane Dynamics.

Authors:  Tomoki Naito; Hiroyuki Takatsu; Rie Miyano; Naoto Takada; Kazuhisa Nakayama; Hye-Won Shin
Journal:  J Biol Chem       Date:  2015-05-06       Impact factor: 5.157

5.  Mapping functional interactions in a heterodimeric phospholipid pump.

Authors:  Catheleyne F Puts; Radhakrishnan Panatala; Hanka Hennrich; Alina Tsareva; Patrick Williamson; Joost C M Holthuis
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6.  Calpain cleaves phospholipid flippase ATP8A1 during apoptosis in platelets.

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7.  Identification of ATP8B1 as a blood-brain barrier-enriched protein.

Authors:  Michael J Haas; Gul N Shah; Luisa M Onstead-Haas; Arshag D Mooradian
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Review 8.  Lipid somersaults: Uncovering the mechanisms of protein-mediated lipid flipping.

Authors:  Thomas Günther Pomorski; Anant K Menon
Journal:  Prog Lipid Res       Date:  2016-08-12       Impact factor: 16.195

9.  Biochemical characterization of P4-ATPase mutations identified in patients with progressive familial intrahepatic cholestasis.

Authors:  Alex Stone; Christopher Chau; Christian Eaton; Emily Foran; Mridu Kapur; Edward Prevatt; Nathan Belkin; David Kerr; Torvald Kohlin; Patrick Williamson
Journal:  J Biol Chem       Date:  2012-10-11       Impact factor: 5.157

10.  Phospholipid flippase activities and substrate specificities of human type IV P-type ATPases localized to the plasma membrane.

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Journal:  J Biol Chem       Date:  2014-10-14       Impact factor: 5.157

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