TWIST1 promotes invasion through mesenchymal change in human glioblastoma

BACKGROUND: Tumor cell invasion into adjacent normal brain is a mesenchymal feature of GBM and a major factor contributing to their dismal outcomes. Therefore, better understandings of mechanisms that promote mesenchymal change in GBM are of great clinical importance to address invasion. We previous...

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Autores principales: Mikheeva, Svetlana A, Mikheev, Andrei M, Petit, Audrey, Beyer, Richard, Oxford, Robert G, Khorasani, Leila, Maxwell, John-Patrick, Glackin, Carlotta A, Wakimoto, Hiroaki, González-Herrero, Inés, Sánchez-García, Isidro, Silber, John R, Horner, Philip J, Rostomily, Robert C
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2010
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2920263/
https://www.ncbi.nlm.nih.gov/pubmed/20646316
http://dx.doi.org/10.1186/1476-4598-9-194
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author Mikheeva, Svetlana A
Mikheev, Andrei M
Petit, Audrey
Beyer, Richard
Oxford, Robert G
Khorasani, Leila
Maxwell, John-Patrick
Glackin, Carlotta A
Wakimoto, Hiroaki
González-Herrero, Inés
Sánchez-García, Isidro
Silber, John R
Horner, Philip J
Rostomily, Robert C
author_facet Mikheeva, Svetlana A
Mikheev, Andrei M
Petit, Audrey
Beyer, Richard
Oxford, Robert G
Khorasani, Leila
Maxwell, John-Patrick
Glackin, Carlotta A
Wakimoto, Hiroaki
González-Herrero, Inés
Sánchez-García, Isidro
Silber, John R
Horner, Philip J
Rostomily, Robert C
author_sort Mikheeva, Svetlana A
collection PubMed
description BACKGROUND: Tumor cell invasion into adjacent normal brain is a mesenchymal feature of GBM and a major factor contributing to their dismal outcomes. Therefore, better understandings of mechanisms that promote mesenchymal change in GBM are of great clinical importance to address invasion. We previously showed that the bHLH transcription factor TWIST1 which orchestrates carcinoma metastasis through an epithelial mesenchymal transition (EMT) is upregulated in GBM and promotes invasion of the SF767 GBM cell line in vitro. RESULTS: To further define TWIST1 functions in GBM we tested the impact of TWIST1 over-expression on invasion in vivo and its impact on gene expression. We found that TWIST1 significantly increased SNB19 and T98G cell line invasion in orthotopic xenotransplants and increased expression of genes in functional categories associated with adhesion, extracellular matrix proteins, cell motility and locomotion, cell migration and actin cytoskeleton organization. Consistent with this TWIST1 reduced cell aggregation, promoted actin cytoskeletal re-organization and enhanced migration and adhesion to fibronectin substrates. Individual genes upregulated by TWIST1 known to promote EMT and/or GBM invasion included SNAI2, MMP2, HGF, FAP and FN1. Distinct from carcinoma EMT, TWIST1 did not generate an E- to N-cadherin "switch" in GBM cell lines. The clinical relevance of putative TWIST target genes SNAI2 and fibroblast activation protein alpha (FAP) identified in vitro was confirmed by their highly correlated expression with TWIST1 in 39 human tumors. The potential therapeutic importance of inhibiting TWIST1 was also shown through a decrease in cell invasion in vitro and growth of GBM stem cells. CONCLUSIONS: Together these studies demonstrated that TWIST1 enhances GBM invasion in concert with mesenchymal change not involving the canonical cadherin switch of carcinoma EMT. Given the recent recognition that mesenchymal change in GBMs is associated with increased malignancy, these findings support the potential therapeutic importance of strategies to subvert TWIST1-mediated mesenchymal change.
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spelling pubmed-29202632010-08-12 TWIST1 promotes invasion through mesenchymal change in human glioblastoma Mikheeva, Svetlana A Mikheev, Andrei M Petit, Audrey Beyer, Richard Oxford, Robert G Khorasani, Leila Maxwell, John-Patrick Glackin, Carlotta A Wakimoto, Hiroaki González-Herrero, Inés Sánchez-García, Isidro Silber, John R Horner, Philip J Rostomily, Robert C Mol Cancer Research BACKGROUND: Tumor cell invasion into adjacent normal brain is a mesenchymal feature of GBM and a major factor contributing to their dismal outcomes. Therefore, better understandings of mechanisms that promote mesenchymal change in GBM are of great clinical importance to address invasion. We previously showed that the bHLH transcription factor TWIST1 which orchestrates carcinoma metastasis through an epithelial mesenchymal transition (EMT) is upregulated in GBM and promotes invasion of the SF767 GBM cell line in vitro. RESULTS: To further define TWIST1 functions in GBM we tested the impact of TWIST1 over-expression on invasion in vivo and its impact on gene expression. We found that TWIST1 significantly increased SNB19 and T98G cell line invasion in orthotopic xenotransplants and increased expression of genes in functional categories associated with adhesion, extracellular matrix proteins, cell motility and locomotion, cell migration and actin cytoskeleton organization. Consistent with this TWIST1 reduced cell aggregation, promoted actin cytoskeletal re-organization and enhanced migration and adhesion to fibronectin substrates. Individual genes upregulated by TWIST1 known to promote EMT and/or GBM invasion included SNAI2, MMP2, HGF, FAP and FN1. Distinct from carcinoma EMT, TWIST1 did not generate an E- to N-cadherin "switch" in GBM cell lines. The clinical relevance of putative TWIST target genes SNAI2 and fibroblast activation protein alpha (FAP) identified in vitro was confirmed by their highly correlated expression with TWIST1 in 39 human tumors. The potential therapeutic importance of inhibiting TWIST1 was also shown through a decrease in cell invasion in vitro and growth of GBM stem cells. CONCLUSIONS: Together these studies demonstrated that TWIST1 enhances GBM invasion in concert with mesenchymal change not involving the canonical cadherin switch of carcinoma EMT. Given the recent recognition that mesenchymal change in GBMs is associated with increased malignancy, these findings support the potential therapeutic importance of strategies to subvert TWIST1-mediated mesenchymal change. BioMed Central 2010-07-20 /pmc/articles/PMC2920263/ /pubmed/20646316 http://dx.doi.org/10.1186/1476-4598-9-194 Text en Copyright ©2010 Mikheeva et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Mikheeva, Svetlana A
Mikheev, Andrei M
Petit, Audrey
Beyer, Richard
Oxford, Robert G
Khorasani, Leila
Maxwell, John-Patrick
Glackin, Carlotta A
Wakimoto, Hiroaki
González-Herrero, Inés
Sánchez-García, Isidro
Silber, John R
Horner, Philip J
Rostomily, Robert C
TWIST1 promotes invasion through mesenchymal change in human glioblastoma
title TWIST1 promotes invasion through mesenchymal change in human glioblastoma
title_full TWIST1 promotes invasion through mesenchymal change in human glioblastoma
title_fullStr TWIST1 promotes invasion through mesenchymal change in human glioblastoma
title_full_unstemmed TWIST1 promotes invasion through mesenchymal change in human glioblastoma
title_short TWIST1 promotes invasion through mesenchymal change in human glioblastoma
title_sort twist1 promotes invasion through mesenchymal change in human glioblastoma
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2920263/
https://www.ncbi.nlm.nih.gov/pubmed/20646316
http://dx.doi.org/10.1186/1476-4598-9-194
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