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Label-Free Segmentation of Co-cultured Cells on a Nanotopographical Gradient

[Image: see text] The function and fate of cells is influenced by many different factors, one of which is surface topography of the support culture substrate. Systematic studies of nanotopography and cell response have typically been limited to single cell types and a small set of topographical vari...

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Autores principales: Reynolds, Paul M., Pedersen, Rasmus H., Stormonth-Darling, John, Dalby, Matthew J., Riehle, Mathis O., Gadegaard, Nikolaj
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2012
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3633255/
https://www.ncbi.nlm.nih.gov/pubmed/23252684
http://dx.doi.org/10.1021/nl304097p
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author Reynolds, Paul M.
Pedersen, Rasmus H.
Stormonth-Darling, John
Dalby, Matthew J.
Riehle, Mathis O.
Gadegaard, Nikolaj
author_facet Reynolds, Paul M.
Pedersen, Rasmus H.
Stormonth-Darling, John
Dalby, Matthew J.
Riehle, Mathis O.
Gadegaard, Nikolaj
author_sort Reynolds, Paul M.
collection PubMed
description [Image: see text] The function and fate of cells is influenced by many different factors, one of which is surface topography of the support culture substrate. Systematic studies of nanotopography and cell response have typically been limited to single cell types and a small set of topographical variations. Here, we show a radical expansion of experimental throughput using automated detection, measurement, and classification of co-cultured cells on a nanopillar array where feature height changes continuously from planar to 250 nm over 9 mm. Individual cells are identified and characterized by more than 200 descriptors, which are used to construct a set of rules for label-free segmentation into individual cell types. Using this approach we can achieve label-free segmentation with 84% confidence across large image data sets and suggest optimized surface parameters for nanostructuring of implant devices such as vascular stents.
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spelling pubmed-36332552013-04-24 Label-Free Segmentation of Co-cultured Cells on a Nanotopographical Gradient Reynolds, Paul M. Pedersen, Rasmus H. Stormonth-Darling, John Dalby, Matthew J. Riehle, Mathis O. Gadegaard, Nikolaj Nano Lett [Image: see text] The function and fate of cells is influenced by many different factors, one of which is surface topography of the support culture substrate. Systematic studies of nanotopography and cell response have typically been limited to single cell types and a small set of topographical variations. Here, we show a radical expansion of experimental throughput using automated detection, measurement, and classification of co-cultured cells on a nanopillar array where feature height changes continuously from planar to 250 nm over 9 mm. Individual cells are identified and characterized by more than 200 descriptors, which are used to construct a set of rules for label-free segmentation into individual cell types. Using this approach we can achieve label-free segmentation with 84% confidence across large image data sets and suggest optimized surface parameters for nanostructuring of implant devices such as vascular stents. American Chemical Society 2012-12-20 2013-02-13 /pmc/articles/PMC3633255/ /pubmed/23252684 http://dx.doi.org/10.1021/nl304097p Text en Copyright © 2012 American Chemical Society
spellingShingle Reynolds, Paul M.
Pedersen, Rasmus H.
Stormonth-Darling, John
Dalby, Matthew J.
Riehle, Mathis O.
Gadegaard, Nikolaj
Label-Free Segmentation of Co-cultured Cells on a Nanotopographical Gradient
title Label-Free Segmentation of Co-cultured Cells on a Nanotopographical Gradient
title_full Label-Free Segmentation of Co-cultured Cells on a Nanotopographical Gradient
title_fullStr Label-Free Segmentation of Co-cultured Cells on a Nanotopographical Gradient
title_full_unstemmed Label-Free Segmentation of Co-cultured Cells on a Nanotopographical Gradient
title_short Label-Free Segmentation of Co-cultured Cells on a Nanotopographical Gradient
title_sort label-free segmentation of co-cultured cells on a nanotopographical gradient
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3633255/
https://www.ncbi.nlm.nih.gov/pubmed/23252684
http://dx.doi.org/10.1021/nl304097p
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