Real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding

Aggressive cellular phenotypes such as uncontrolled proliferation and increased migration capacity engender cellular transformation, malignancy and metastasis. While genetic mutations are undisputed drivers of cancer initiation and progression, it is increasingly accepted that external factors are a...

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Autores principales: Pratt, Stephen J.P., Hernández-Ochoa, Erick O., Lee, Rachel M., Ory, Eleanor C., Lyons, James S., Joca, Humberto C., Johnson, Ashley, Thompson, Keyata, Bailey, Patrick, Lee, Cornell J., Mathias, Trevor, Vitolo, Michele I., Trudeau, Matt, Stains, Joseph P., Ward, Christopher W., Schneider, Martin F., Martin, Stuart S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5982755/
https://www.ncbi.nlm.nih.gov/pubmed/29861849
http://dx.doi.org/10.18632/oncotarget.25186
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author Pratt, Stephen J.P.
Hernández-Ochoa, Erick O.
Lee, Rachel M.
Ory, Eleanor C.
Lyons, James S.
Joca, Humberto C.
Johnson, Ashley
Thompson, Keyata
Bailey, Patrick
Lee, Cornell J.
Mathias, Trevor
Vitolo, Michele I.
Trudeau, Matt
Stains, Joseph P.
Ward, Christopher W.
Schneider, Martin F.
Martin, Stuart S.
author_facet Pratt, Stephen J.P.
Hernández-Ochoa, Erick O.
Lee, Rachel M.
Ory, Eleanor C.
Lyons, James S.
Joca, Humberto C.
Johnson, Ashley
Thompson, Keyata
Bailey, Patrick
Lee, Cornell J.
Mathias, Trevor
Vitolo, Michele I.
Trudeau, Matt
Stains, Joseph P.
Ward, Christopher W.
Schneider, Martin F.
Martin, Stuart S.
author_sort Pratt, Stephen J.P.
collection PubMed
description Aggressive cellular phenotypes such as uncontrolled proliferation and increased migration capacity engender cellular transformation, malignancy and metastasis. While genetic mutations are undisputed drivers of cancer initiation and progression, it is increasingly accepted that external factors are also playing a major role. Two recently studied modulators of breast cancer are changes in the cellular mechanical microenvironment and alterations in calcium homeostasis. While many studies investigate these factors separately in breast cancer cells, very few do so in combination. This current work sets a foundation to explore mechano-calcium relationships driving malignant progression in breast cancer. Utilizing real-time imaging of an in vitro scratch assay, we were able to resolve mechanically-sensitive calcium signaling in human breast cancer cells. We observed rapid initiation of intracellular calcium elevations within seconds in cells at the immediate wound edge, followed by a time-dependent increase in calcium in cells at distances up to 500μm from the scratch wound. Calcium signaling to neighboring cells away from the wound edge returned to baseline within seconds. Calcium elevations at the wound edge however, persisted for up to 50 minutes. Rigorous quantification showed that extracellular calcium was necessary for persistent calcium elevation at the wound edge, but intercellular signal propagation was dependent on internal calcium stores. In addition, intercellular signaling required extracellular ATP and activation of P2Y(2) receptors. Through comparison of scratch-induced signaling from multiple cell lines, we report drastic reductions in response from aggressively tumorigenic and metastatic cells. The real-time scratch assay established here provides quantitative data on the molecular mechanisms that support rapid scratch-induced calcium signaling in breast cancer cells. These mechanisms now provide a clear framework for investigating which short-term calcium signals promote long-term changes in cancer cell biology.
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spelling pubmed-59827552018-06-01 Real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding Pratt, Stephen J.P. Hernández-Ochoa, Erick O. Lee, Rachel M. Ory, Eleanor C. Lyons, James S. Joca, Humberto C. Johnson, Ashley Thompson, Keyata Bailey, Patrick Lee, Cornell J. Mathias, Trevor Vitolo, Michele I. Trudeau, Matt Stains, Joseph P. Ward, Christopher W. Schneider, Martin F. Martin, Stuart S. Oncotarget Research Paper Aggressive cellular phenotypes such as uncontrolled proliferation and increased migration capacity engender cellular transformation, malignancy and metastasis. While genetic mutations are undisputed drivers of cancer initiation and progression, it is increasingly accepted that external factors are also playing a major role. Two recently studied modulators of breast cancer are changes in the cellular mechanical microenvironment and alterations in calcium homeostasis. While many studies investigate these factors separately in breast cancer cells, very few do so in combination. This current work sets a foundation to explore mechano-calcium relationships driving malignant progression in breast cancer. Utilizing real-time imaging of an in vitro scratch assay, we were able to resolve mechanically-sensitive calcium signaling in human breast cancer cells. We observed rapid initiation of intracellular calcium elevations within seconds in cells at the immediate wound edge, followed by a time-dependent increase in calcium in cells at distances up to 500μm from the scratch wound. Calcium signaling to neighboring cells away from the wound edge returned to baseline within seconds. Calcium elevations at the wound edge however, persisted for up to 50 minutes. Rigorous quantification showed that extracellular calcium was necessary for persistent calcium elevation at the wound edge, but intercellular signal propagation was dependent on internal calcium stores. In addition, intercellular signaling required extracellular ATP and activation of P2Y(2) receptors. Through comparison of scratch-induced signaling from multiple cell lines, we report drastic reductions in response from aggressively tumorigenic and metastatic cells. The real-time scratch assay established here provides quantitative data on the molecular mechanisms that support rapid scratch-induced calcium signaling in breast cancer cells. These mechanisms now provide a clear framework for investigating which short-term calcium signals promote long-term changes in cancer cell biology. Impact Journals LLC 2018-05-18 /pmc/articles/PMC5982755/ /pubmed/29861849 http://dx.doi.org/10.18632/oncotarget.25186 Text en Copyright: © 2018 Pratt et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License 3.0 (http://creativecommons.org/licenses/by/3.0/) (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Pratt, Stephen J.P.
Hernández-Ochoa, Erick O.
Lee, Rachel M.
Ory, Eleanor C.
Lyons, James S.
Joca, Humberto C.
Johnson, Ashley
Thompson, Keyata
Bailey, Patrick
Lee, Cornell J.
Mathias, Trevor
Vitolo, Michele I.
Trudeau, Matt
Stains, Joseph P.
Ward, Christopher W.
Schneider, Martin F.
Martin, Stuart S.
Real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding
title Real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding
title_full Real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding
title_fullStr Real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding
title_full_unstemmed Real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding
title_short Real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding
title_sort real-time scratch assay reveals mechanisms of early calcium signaling in breast cancer cells in response to wounding
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5982755/
https://www.ncbi.nlm.nih.gov/pubmed/29861849
http://dx.doi.org/10.18632/oncotarget.25186
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