Literature DB >> 21374596

AKAP350 Is involved in the development of apical "canalicular" structures in hepatic cells HepG2.

Stella M Mattaloni1, Elena Kolobova, Cristián Favre, Raúl A Marinelli, James R Goldenring, Maria C Larocca.   

Abstract

Hepatocytes are epithelial cells whose apical poles constitute the bile canaliculi. The establishment and maintenance of canalicular poles is a finely regulated process that dictates the efficiency of primary bile secretion. Protein kinase A (PKA) modulates this process at different levels. AKAP350 is an A-kinase anchoring protein that scaffolds protein complexes involved in modulating the dynamic structures of the Golgi apparatus and microtubule cytoskeleton, facilitating microtubule nucleation at this organelle. In this study, we evaluated whether AKAP350 is involved in the development of bile canaliculi-like structures in hepatocyte derived HepG2 cells. We found that AKAP350 recruits PKA to the centrosomes and Golgi apparatus in HepG2 cells. De-localization of AKAP350 from these organelles led to reduced apical cell polarization. A decrease in AKAP350 expression inhibited the formation of canalicular structures and impaired F-actin organization at canalicular poles. Furthermore, loss of AKAP350 expression led to diminished polarized expression of the p-glycoprotein (MDR1/ABCB1) at the apical "canalicular" membrane. AKAP350 knock down effects on canalicular structures formation and actin organization could be mimicked by inhibition of Golgi microtubule nucleation by depletion of CLIP associated proteins (CLASPs). Our data reveal that AKAP350 participates in mechanisms which determine the development of canalicular structures as well as accurate canalicular expression of distinct proteins and actin organization, and provide evidence on the involvement of Golgi microtubule nucleation in hepatocyte apical polarization.
Copyright © 2011 Wiley Periodicals, Inc.

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Year:  2012        PMID: 21374596      PMCID: PMC3899033          DOI: 10.1002/jcp.22713

Source DB:  PubMed          Journal:  J Cell Physiol        ISSN: 0021-9541            Impact factor:   6.384


  46 in total

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Journal:  HPB (Oxford)       Date:  2013-09-24       Impact factor: 3.647

3.  Microtubules regulate brush border formation.

Authors:  Facundo M Tonucci; Anabela Ferretti; Evangelina Almada; Pamela Cribb; Rodrigo Vena; Florencia Hidalgo; Cristián Favre; Matt J Tyska; Irina Kaverina; Maria C Larocca
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4.  Centrosomal AKAP350 and CIP4 act in concert to define the polarized localization of the centrosome and Golgi in migratory cells.

Authors:  Facundo M Tonucci; Florencia Hidalgo; Anabela Ferretti; Evangelina Almada; Cristián Favre; James R Goldenring; Irina Kaverina; Arlinet Kierbel; M Cecilia Larocca
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5.  AMPK and PKA interaction in the regulation of survival of liver cancer cells subjected to glucose starvation.

Authors:  Anabela C Ferretti; Facundo M Tonucci; Florencia Hidalgo; Evangelina Almada; Maria C Larocca; Cristián Favre
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6.  RSK1 protects P-glycoprotein/ABCB1 against ubiquitin-proteasomal degradation by downregulating the ubiquitin-conjugating enzyme E2 R1.

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7.  Akap350 Recruits Eb1 to The Spindle Poles, Ensuring Proper Spindle Orientation and Lumen Formation in 3d Epithelial Cell Cultures.

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8.  Metformin and glucose starvation decrease the migratory ability of hepatocellular carcinoma cells: targeting AMPK activation to control migration.

Authors:  Anabela C Ferretti; Florencia Hidalgo; Facundo M Tonucci; Evangelina Almada; Alejandro Pariani; María C Larocca; Cristián Favre
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9.  Centrosomal AKAP350 modulates the G1/S transition.

Authors:  Stella M Mattaloni; Anabela C Ferretti; Facundo M Tonucci; Cristián Favre; James R Goldenring; M Cecilia Larocca
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  9 in total

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