Roles of the phosphatase POPX in the regulation of cell signalling and cell morphology.

Rho GTPases and their downstream effectors regulate changes in the actin cytoskeleton that underlie cell motility and adhesion. They also participate in the regulation of gene transcription with RhoA activating serum response factor (SRF) mediated transcription from the serum response element (SRE)....

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Main Author: Koh, Cheng Gee
Other Authors: School of Biological Sciences
Format: Research Report
Language:English
Published: 2009
Subjects:
Online Access:http://hdl.handle.net/10356/17221
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-172212023-02-28T17:58:29Z Roles of the phosphatase POPX in the regulation of cell signalling and cell morphology. Koh, Cheng Gee School of Biological Sciences DRNTU::Science::Biological sciences::Cytology Rho GTPases and their downstream effectors regulate changes in the actin cytoskeleton that underlie cell motility and adhesion. They also participate in the regulation of gene transcription with RhoA activating serum response factor (SRF) mediated transcription from the serum response element (SRE). SRF-mediated transcription is also promoted by indentified a family of PP2C phosphatases, POPXs, which can dephosphorylate Cdc42/Rac-actived kinase PAK and down regulate its enzymatic and actin cytoskeletal activity. We now report that POPX interacts with the formin protein mDia. This interaction is enhanced when mDia is activated by RhoA. The binding of POPX to mDia-containing complex greatly decreases the ability of mDia to activate transcription from SRE. We propose that the interaction between mDia and POPX2 serves to regulate both the actin cytokeleton and SRF-mediated transcription, and to link Cdc42/Rac with RhoA pathways. RG 148/06 2009-06-01T08:50:41Z 2009-06-01T08:50:41Z 2008 2008 Research Report http://hdl.handle.net/10356/17221 en 26 p. application/pdf
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic DRNTU::Science::Biological sciences::Cytology
spellingShingle DRNTU::Science::Biological sciences::Cytology
Koh, Cheng Gee
Roles of the phosphatase POPX in the regulation of cell signalling and cell morphology.
description Rho GTPases and their downstream effectors regulate changes in the actin cytoskeleton that underlie cell motility and adhesion. They also participate in the regulation of gene transcription with RhoA activating serum response factor (SRF) mediated transcription from the serum response element (SRE). SRF-mediated transcription is also promoted by indentified a family of PP2C phosphatases, POPXs, which can dephosphorylate Cdc42/Rac-actived kinase PAK and down regulate its enzymatic and actin cytoskeletal activity. We now report that POPX interacts with the formin protein mDia. This interaction is enhanced when mDia is activated by RhoA. The binding of POPX to mDia-containing complex greatly decreases the ability of mDia to activate transcription from SRE. We propose that the interaction between mDia and POPX2 serves to regulate both the actin cytokeleton and SRF-mediated transcription, and to link Cdc42/Rac with RhoA pathways.
author2 School of Biological Sciences
author_facet School of Biological Sciences
Koh, Cheng Gee
format Research Report
author Koh, Cheng Gee
author_sort Koh, Cheng Gee
title Roles of the phosphatase POPX in the regulation of cell signalling and cell morphology.
title_short Roles of the phosphatase POPX in the regulation of cell signalling and cell morphology.
title_full Roles of the phosphatase POPX in the regulation of cell signalling and cell morphology.
title_fullStr Roles of the phosphatase POPX in the regulation of cell signalling and cell morphology.
title_full_unstemmed Roles of the phosphatase POPX in the regulation of cell signalling and cell morphology.
title_sort roles of the phosphatase popx in the regulation of cell signalling and cell morphology.
publishDate 2009
url http://hdl.handle.net/10356/17221
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