Fascin Is Regulated by Slug, Promotes Progression of Pancreatic Cancer in Mice, and Is Associated With Patient Outcomes

BACKGROUND & AIMS: Pancreatic ductal adenocarcinoma (PDAC) is often lethal because it is highly invasive and metastasizes rapidly. The actin-bundling protein fascin has been identified as a biomarker of invasive and advanced PDAC and regulates cell migration and invasion in vitro. We investigate...

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Autores principales: Li, Ang, Morton, Jennifer P., Ma, YaFeng, Karim, Saadia A., Zhou, Yan, Faller, William J., Woodham, Emma F., Morris, Hayley T., Stevenson, Richard P., Juin, Amelie, Jamieson, Nigel B., MacKay, Colin J., Carter, C. Ross, Leung, Hing Y., Yamashiro, Shigeko, Blyth, Karen, Sansom, Owen J., Machesky, Laura M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: W.B. Saunders 2014
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4000441/
https://www.ncbi.nlm.nih.gov/pubmed/24462734
http://dx.doi.org/10.1053/j.gastro.2014.01.046
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author Li, Ang
Morton, Jennifer P.
Ma, YaFeng
Karim, Saadia A.
Zhou, Yan
Faller, William J.
Woodham, Emma F.
Morris, Hayley T.
Stevenson, Richard P.
Juin, Amelie
Jamieson, Nigel B.
MacKay, Colin J.
Carter, C. Ross
Leung, Hing Y.
Yamashiro, Shigeko
Blyth, Karen
Sansom, Owen J.
Machesky, Laura M.
author_facet Li, Ang
Morton, Jennifer P.
Ma, YaFeng
Karim, Saadia A.
Zhou, Yan
Faller, William J.
Woodham, Emma F.
Morris, Hayley T.
Stevenson, Richard P.
Juin, Amelie
Jamieson, Nigel B.
MacKay, Colin J.
Carter, C. Ross
Leung, Hing Y.
Yamashiro, Shigeko
Blyth, Karen
Sansom, Owen J.
Machesky, Laura M.
author_sort Li, Ang
collection PubMed
description BACKGROUND & AIMS: Pancreatic ductal adenocarcinoma (PDAC) is often lethal because it is highly invasive and metastasizes rapidly. The actin-bundling protein fascin has been identified as a biomarker of invasive and advanced PDAC and regulates cell migration and invasion in vitro. We investigated fascin expression and its role in PDAC progression in mice. METHODS: We used KRas(G12D) p53(R172H) Pdx1-Cre (KPC) mice to investigate the effects of fascin deficiency on development of pancreatic intraepithelial neoplasia (PanIn), PDAC, and metastasis. We measured levels of fascin in PDAC cell lines and 122 human resected PDAC samples, along with normal ductal and acinar tissues; we associated levels with patient outcomes. RESULTS: Pancreatic ducts and acini from control mice and early-stage PanINs from KPC mice were negative for fascin, but approximately 6% of PanIN3 and 100% of PDAC expressed fascin. Fascin-deficient KRas(G12D) p53(R172H) Pdx1-Cre mice had longer survival times, delayed onset of PDAC, and a lower PDAC tumor burdens than KPC mice; loss of fascin did not affect invasion of PDAC into bowel or peritoneum in mice. Levels of slug and fascin correlated in PDAC cells; slug was found to regulate transcription of Fascin along with the epithelial−mesenchymal transition. In PDAC cell lines and cells from mice, fascin concentrated in filopodia and was required for their assembly and turnover. Fascin promoted intercalation of filopodia into mesothelial cell layers and cell invasion. Nearly all human PDAC samples expressed fascin, and higher fascin histoscores correlated with poor outcomes, vascular invasion, and time to recurrence. CONCLUSIONS: The actin-bundling protein fascin is regulated by slug and involved in late-stage PanIN and PDAC formation in mice. Fascin appears to promote formation of filopodia and invasive activities of PDAC cells. Its levels in human PDAC correlate with outcomes and time to recurrence, indicating it might be a marker or therapeutic target for pancreatic cancer.
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spelling pubmed-40004412014-05-01 Fascin Is Regulated by Slug, Promotes Progression of Pancreatic Cancer in Mice, and Is Associated With Patient Outcomes Li, Ang Morton, Jennifer P. Ma, YaFeng Karim, Saadia A. Zhou, Yan Faller, William J. Woodham, Emma F. Morris, Hayley T. Stevenson, Richard P. Juin, Amelie Jamieson, Nigel B. MacKay, Colin J. Carter, C. Ross Leung, Hing Y. Yamashiro, Shigeko Blyth, Karen Sansom, Owen J. Machesky, Laura M. Gastroenterology Original Research BACKGROUND & AIMS: Pancreatic ductal adenocarcinoma (PDAC) is often lethal because it is highly invasive and metastasizes rapidly. The actin-bundling protein fascin has been identified as a biomarker of invasive and advanced PDAC and regulates cell migration and invasion in vitro. We investigated fascin expression and its role in PDAC progression in mice. METHODS: We used KRas(G12D) p53(R172H) Pdx1-Cre (KPC) mice to investigate the effects of fascin deficiency on development of pancreatic intraepithelial neoplasia (PanIn), PDAC, and metastasis. We measured levels of fascin in PDAC cell lines and 122 human resected PDAC samples, along with normal ductal and acinar tissues; we associated levels with patient outcomes. RESULTS: Pancreatic ducts and acini from control mice and early-stage PanINs from KPC mice were negative for fascin, but approximately 6% of PanIN3 and 100% of PDAC expressed fascin. Fascin-deficient KRas(G12D) p53(R172H) Pdx1-Cre mice had longer survival times, delayed onset of PDAC, and a lower PDAC tumor burdens than KPC mice; loss of fascin did not affect invasion of PDAC into bowel or peritoneum in mice. Levels of slug and fascin correlated in PDAC cells; slug was found to regulate transcription of Fascin along with the epithelial−mesenchymal transition. In PDAC cell lines and cells from mice, fascin concentrated in filopodia and was required for their assembly and turnover. Fascin promoted intercalation of filopodia into mesothelial cell layers and cell invasion. Nearly all human PDAC samples expressed fascin, and higher fascin histoscores correlated with poor outcomes, vascular invasion, and time to recurrence. CONCLUSIONS: The actin-bundling protein fascin is regulated by slug and involved in late-stage PanIN and PDAC formation in mice. Fascin appears to promote formation of filopodia and invasive activities of PDAC cells. Its levels in human PDAC correlate with outcomes and time to recurrence, indicating it might be a marker or therapeutic target for pancreatic cancer. W.B. Saunders 2014-05 /pmc/articles/PMC4000441/ /pubmed/24462734 http://dx.doi.org/10.1053/j.gastro.2014.01.046 Text en © 2014 AGA Institute. Published by Elsevier Inc. All rights reserved. https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Original Research
Li, Ang
Morton, Jennifer P.
Ma, YaFeng
Karim, Saadia A.
Zhou, Yan
Faller, William J.
Woodham, Emma F.
Morris, Hayley T.
Stevenson, Richard P.
Juin, Amelie
Jamieson, Nigel B.
MacKay, Colin J.
Carter, C. Ross
Leung, Hing Y.
Yamashiro, Shigeko
Blyth, Karen
Sansom, Owen J.
Machesky, Laura M.
Fascin Is Regulated by Slug, Promotes Progression of Pancreatic Cancer in Mice, and Is Associated With Patient Outcomes
title Fascin Is Regulated by Slug, Promotes Progression of Pancreatic Cancer in Mice, and Is Associated With Patient Outcomes
title_full Fascin Is Regulated by Slug, Promotes Progression of Pancreatic Cancer in Mice, and Is Associated With Patient Outcomes
title_fullStr Fascin Is Regulated by Slug, Promotes Progression of Pancreatic Cancer in Mice, and Is Associated With Patient Outcomes
title_full_unstemmed Fascin Is Regulated by Slug, Promotes Progression of Pancreatic Cancer in Mice, and Is Associated With Patient Outcomes
title_short Fascin Is Regulated by Slug, Promotes Progression of Pancreatic Cancer in Mice, and Is Associated With Patient Outcomes
title_sort fascin is regulated by slug, promotes progression of pancreatic cancer in mice, and is associated with patient outcomes
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4000441/
https://www.ncbi.nlm.nih.gov/pubmed/24462734
http://dx.doi.org/10.1053/j.gastro.2014.01.046
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