Literature DB >> 25483195

POPX2 phosphatase regulates cell polarity and centrosome placement.

Jing-Ling Hoon1, Hoi-Yeung Li, Cheng-Gee Koh.   

Abstract

Proper centrosome positioning is critical for many cellular functions, such as cell migration and maintenance of polarity. During wound healing, fibroblasts orient their centrosomes such that they face the wound edge. The centrosome orientation determines the direction of cells' migration so that they can close the wound effectively. In this study, we investigated the regulation of centrosome polarization and have identified the phosphatase POPX2 as an important regulator of centrosome orientation. We found that POPX2 inhibits centrosome centration, but not rearward nuclear movement, by regulating multiple proteins that function in centrosome positioning. High POPX2 levels result in reduced motility of the kinesin-2 motor, which, in turn, inhibits the transport of N-cadherin to the cell periphery and cell junctions. Loss of N-cadherin localization to the cell membrane affects the localization of focal adhesions and perturbs CDC42-Par6/PKCζ signaling. In addition, overexpression of POPX2 also results in a loss of Par3 localization to the cell periphery and reduced levels of LIC2 (dynein light intermediate chain 2), leading to defects in microtubule tethering and dynamics at cell-cell contacts. Therefore, POPX2 functions as a regulator of signaling pathways to modulate the positioning of centrosome in fibroblast during wound healing.

Entities:  

Keywords:  Kinesin-2 motor; N-cadherin; POPX2 phosphatase; Par3; calcium/calmodulin kinase; centrosome; dynein light intermediate chain 2

Mesh:

Substances:

Year:  2014        PMID: 25483195      PMCID: PMC4128889          DOI: 10.4161/cc.29421

Source DB:  PubMed          Journal:  Cell Cycle        ISSN: 1551-4005            Impact factor:   4.534


  26 in total

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3.  Integrin-mediated activation of Cdc42 controls cell polarity in migrating astrocytes through PKCzeta.

Authors:  S Etienne-Manneville; A Hall
Journal:  Cell       Date:  2001-08-24       Impact factor: 41.582

4.  The p21-activated kinase PAK is negatively regulated by POPX1 and POPX2, a pair of serine/threonine phosphatases of the PP2C family.

Authors:  Cheng-Gee Koh; E-Jean Tan; Edward Manser; Louis Lim
Journal:  Curr Biol       Date:  2002-02-19       Impact factor: 10.834

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7.  Cdc42, dynein, and dynactin regulate MTOC reorientation independent of Rho-regulated microtubule stabilization.

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8.  Regulation of the multifunctional Ca2+/calmodulin-dependent protein kinase II by the PP2C phosphatase PPM1F in fibroblasts.

Authors:  Bohdan P Harvey; Satnam S Banga; Harvey L Ozer
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9.  Localized cdc42 activation, detected using a novel assay, mediates microtubule organizing center positioning in endothelial cells in response to fluid shear stress.

Authors:  Eleni Tzima; William B Kiosses; Miguel A del Pozo; Martin Alexander Schwartz
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10.  Direct interaction of pericentrin with cytoplasmic dynein light intermediate chain contributes to mitotic spindle organization.

Authors:  A Purohit; S H Tynan; R Vallee; S J Doxsey
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  7 in total

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Review 2.  The effects of locomotion on bone marrow mesenchymal stem cell fate: insight into mechanical regulation and bone formation.

Authors:  Yuanxiu Sun; Yu Yuan; Wei Wu; Le Lei; Lingli Zhang
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3.  Protein phosphatase Mg2+/Mn2+ dependent 1F promotes smoking-induced breast cancer by inactivating phosphorylated-p53-induced signals.

Authors:  Shih-Hsin Tu; Yin-Ching Lin; Chi-Cheng Huang; Po-Sheng Yang; Hui-Wen Chang; Chien-Hsi Chang; Chih-Hsiung Wu; Li-Ching Chen; Yuan-Soon Ho
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4.  POPX2 is a novel LATS phosphatase that regulates the Hippo pathway.

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Review 5.  Partners in crime: POPX2 phosphatase and its interacting proteins in cancer.

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Journal:  Cell Death Dis       Date:  2020-10-09       Impact factor: 8.469

Review 6.  Protein phosphatases in TLR signaling.

Authors:  Clovis H T Seumen; Tanja M Grimm; Christof R Hauck
Journal:  Cell Commun Signal       Date:  2021-04-21       Impact factor: 5.712

7.  POPX2 phosphatase regulates apoptosis through the TAK1-IKK-NF-κB pathway.

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Journal:  Cell Death Dis       Date:  2017-09-14       Impact factor: 8.469

  7 in total

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