Hax-1 is required for Rac1-Cortactin interaction and ovarian carcinoma cell migration

Hax-1 is a multifunctional protein, which is involved in diverse cellular signaling pathways including tumor cell survival and migration. We have shown previously that cell migration stimulated by the oncogenic G protein, G(13,) requires Hax-1 for the formation of a functional complex involving Gα(1...

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Autores principales: Gomathinayagam, Rohini, Muralidharan, Jayaraman, Ha, Ji Hee, Varadarajalu, Lakshmi, Dhanasekaran, Danny N.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4091533/
https://www.ncbi.nlm.nih.gov/pubmed/25053987
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author Gomathinayagam, Rohini
Muralidharan, Jayaraman
Ha, Ji Hee
Varadarajalu, Lakshmi
Dhanasekaran, Danny N.
author_facet Gomathinayagam, Rohini
Muralidharan, Jayaraman
Ha, Ji Hee
Varadarajalu, Lakshmi
Dhanasekaran, Danny N.
author_sort Gomathinayagam, Rohini
collection PubMed
description Hax-1 is a multifunctional protein, which is involved in diverse cellular signaling pathways including tumor cell survival and migration. We have shown previously that cell migration stimulated by the oncogenic G protein, G(13,) requires Hax-1 for the formation of a functional complex involving Gα(13), Rac1, and cortactin. However, the role of Hax-1 in cancer cell migration or its role in Rac1-cortactin complex formation, which is known to be required for such migration remains to be characterized. Results focused on resolving the role of Hax-1 in ovarian cancer pathophysiology indicate that Hax-1 is overexpressed in ovarian cancer cells and the silencing of Hax-1 inhibits lysophosphatidic acid (LPA)- or fetal bovine serum-stimulated migration of these cells. In addition, silencing of Hax-1 greatly reduces Rac1-cortactin interaction and their colocalization in SKOV3 cells. Mapping the structural domains of Hax-1 indicates that it interacts with cortactin via domains spanning amino acids 1 to 56 (Hax-D1) and amino acids 113 to 168 (Hax-D3). Much weaker interaction with cortactin was also observed with the region of Hax-1 spanning amino acids 169 – 224 (Hax-D4). Similar mapping of Hax-1 domains involved in Rac1 interaction indicates that it associates with Rac1 via two primary domains spanning amino acids 57 to 112 (Hax-D2) and 169 to 224 (Hax-D4). Furthermore, expression of either of these domains inhibits LPA-mediated migration of SKOV3 cells, possibly through their ability to exert competitive inhibition on endogenous Hax-1-Rac1 and/or Hax-1-cortactin interaction. More significantly, expression of Hax-D4 drastically reduces Rac1-cortactin colocalization in SKOV3 cells along with an attenuation of LPA-stimulated migration. Thus our results presented here describe for the first time that Hax-1 interaction is required for the association between Rac1 and cortactin and that these multiple interactions are required for the LPA-stimulated migration of SKOV3 ovarian cancer cells.
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spelling pubmed-40915332014-07-22 Hax-1 is required for Rac1-Cortactin interaction and ovarian carcinoma cell migration Gomathinayagam, Rohini Muralidharan, Jayaraman Ha, Ji Hee Varadarajalu, Lakshmi Dhanasekaran, Danny N. Genes Cancer Research Paper Hax-1 is a multifunctional protein, which is involved in diverse cellular signaling pathways including tumor cell survival and migration. We have shown previously that cell migration stimulated by the oncogenic G protein, G(13,) requires Hax-1 for the formation of a functional complex involving Gα(13), Rac1, and cortactin. However, the role of Hax-1 in cancer cell migration or its role in Rac1-cortactin complex formation, which is known to be required for such migration remains to be characterized. Results focused on resolving the role of Hax-1 in ovarian cancer pathophysiology indicate that Hax-1 is overexpressed in ovarian cancer cells and the silencing of Hax-1 inhibits lysophosphatidic acid (LPA)- or fetal bovine serum-stimulated migration of these cells. In addition, silencing of Hax-1 greatly reduces Rac1-cortactin interaction and their colocalization in SKOV3 cells. Mapping the structural domains of Hax-1 indicates that it interacts with cortactin via domains spanning amino acids 1 to 56 (Hax-D1) and amino acids 113 to 168 (Hax-D3). Much weaker interaction with cortactin was also observed with the region of Hax-1 spanning amino acids 169 – 224 (Hax-D4). Similar mapping of Hax-1 domains involved in Rac1 interaction indicates that it associates with Rac1 via two primary domains spanning amino acids 57 to 112 (Hax-D2) and 169 to 224 (Hax-D4). Furthermore, expression of either of these domains inhibits LPA-mediated migration of SKOV3 cells, possibly through their ability to exert competitive inhibition on endogenous Hax-1-Rac1 and/or Hax-1-cortactin interaction. More significantly, expression of Hax-D4 drastically reduces Rac1-cortactin colocalization in SKOV3 cells along with an attenuation of LPA-stimulated migration. Thus our results presented here describe for the first time that Hax-1 interaction is required for the association between Rac1 and cortactin and that these multiple interactions are required for the LPA-stimulated migration of SKOV3 ovarian cancer cells. Impact Journals LLC 2014-03 /pmc/articles/PMC4091533/ /pubmed/25053987 Text en Copyright: © 2014 Gomathinayagam et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Gomathinayagam, Rohini
Muralidharan, Jayaraman
Ha, Ji Hee
Varadarajalu, Lakshmi
Dhanasekaran, Danny N.
Hax-1 is required for Rac1-Cortactin interaction and ovarian carcinoma cell migration
title Hax-1 is required for Rac1-Cortactin interaction and ovarian carcinoma cell migration
title_full Hax-1 is required for Rac1-Cortactin interaction and ovarian carcinoma cell migration
title_fullStr Hax-1 is required for Rac1-Cortactin interaction and ovarian carcinoma cell migration
title_full_unstemmed Hax-1 is required for Rac1-Cortactin interaction and ovarian carcinoma cell migration
title_short Hax-1 is required for Rac1-Cortactin interaction and ovarian carcinoma cell migration
title_sort hax-1 is required for rac1-cortactin interaction and ovarian carcinoma cell migration
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4091533/
https://www.ncbi.nlm.nih.gov/pubmed/25053987
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