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Microenvironmental Geometry Guides Platelet Adhesion and Spreading: A Quantitative Analysis at the Single Cell Level

To activate clot formation and maintain hemostasis, platelets adhere and spread onto sites of vascular injury. Although this process is well-characterized biochemically, how the physical and spatial cues in the microenvironment affect platelet adhesion and spreading remain unclear. In this study, we...

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Autores principales: Kita, Ashley, Sakurai, Yumiko, Myers, David R., Rounsevell, Ross, Huang, James N., Seok, Tae Joon, Yu, Kyoungsik, Wu, Ming C., Fletcher, Daniel A., Lam, Wilbur A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3197646/
https://www.ncbi.nlm.nih.gov/pubmed/22028878
http://dx.doi.org/10.1371/journal.pone.0026437
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author Kita, Ashley
Sakurai, Yumiko
Myers, David R.
Rounsevell, Ross
Huang, James N.
Seok, Tae Joon
Yu, Kyoungsik
Wu, Ming C.
Fletcher, Daniel A.
Lam, Wilbur A.
author_facet Kita, Ashley
Sakurai, Yumiko
Myers, David R.
Rounsevell, Ross
Huang, James N.
Seok, Tae Joon
Yu, Kyoungsik
Wu, Ming C.
Fletcher, Daniel A.
Lam, Wilbur A.
author_sort Kita, Ashley
collection PubMed
description To activate clot formation and maintain hemostasis, platelets adhere and spread onto sites of vascular injury. Although this process is well-characterized biochemically, how the physical and spatial cues in the microenvironment affect platelet adhesion and spreading remain unclear. In this study, we applied deep UV photolithography and protein micro/nanostamping to quantitatively investigate and characterize the spatial guidance of platelet spreading at the single cell level and with nanoscale resolution. Platelets adhered to and spread only onto micropatterned collagen or fibrinogen surfaces and followed the microenvironmental geometry with high fidelity and with single micron precision. Using micropatterned lines of different widths, we determined that platelets are able to conform to micropatterned stripes as thin as 0.6 µm and adopt a maximum aspect ratio of 19 on those protein patterns. Interestingly, platelets were also able to span and spread over non-patterned regions of up to 5 µm, a length consistent with that of maximally extended filopodia. This process appears to be mediated by platelet filopodia that are sensitive to spatial cues. Finally, we observed that microenvironmental geometry directly affects platelet biology, such as the spatial organization and distribution of the platelet actin cytoskeleton. Our data demonstrate that platelet spreading is a finely-tuned and spatially-guided process in which spatial cues directly influence the biological aspects of how clot formation is regulated.
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spelling pubmed-31976462011-10-25 Microenvironmental Geometry Guides Platelet Adhesion and Spreading: A Quantitative Analysis at the Single Cell Level Kita, Ashley Sakurai, Yumiko Myers, David R. Rounsevell, Ross Huang, James N. Seok, Tae Joon Yu, Kyoungsik Wu, Ming C. Fletcher, Daniel A. Lam, Wilbur A. PLoS One Research Article To activate clot formation and maintain hemostasis, platelets adhere and spread onto sites of vascular injury. Although this process is well-characterized biochemically, how the physical and spatial cues in the microenvironment affect platelet adhesion and spreading remain unclear. In this study, we applied deep UV photolithography and protein micro/nanostamping to quantitatively investigate and characterize the spatial guidance of platelet spreading at the single cell level and with nanoscale resolution. Platelets adhered to and spread only onto micropatterned collagen or fibrinogen surfaces and followed the microenvironmental geometry with high fidelity and with single micron precision. Using micropatterned lines of different widths, we determined that platelets are able to conform to micropatterned stripes as thin as 0.6 µm and adopt a maximum aspect ratio of 19 on those protein patterns. Interestingly, platelets were also able to span and spread over non-patterned regions of up to 5 µm, a length consistent with that of maximally extended filopodia. This process appears to be mediated by platelet filopodia that are sensitive to spatial cues. Finally, we observed that microenvironmental geometry directly affects platelet biology, such as the spatial organization and distribution of the platelet actin cytoskeleton. Our data demonstrate that platelet spreading is a finely-tuned and spatially-guided process in which spatial cues directly influence the biological aspects of how clot formation is regulated. Public Library of Science 2011-10-20 /pmc/articles/PMC3197646/ /pubmed/22028878 http://dx.doi.org/10.1371/journal.pone.0026437 Text en Kita et al. http://creativecommons.org/licenses/by/4.0/ 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 properly credited.
spellingShingle Research Article
Kita, Ashley
Sakurai, Yumiko
Myers, David R.
Rounsevell, Ross
Huang, James N.
Seok, Tae Joon
Yu, Kyoungsik
Wu, Ming C.
Fletcher, Daniel A.
Lam, Wilbur A.
Microenvironmental Geometry Guides Platelet Adhesion and Spreading: A Quantitative Analysis at the Single Cell Level
title Microenvironmental Geometry Guides Platelet Adhesion and Spreading: A Quantitative Analysis at the Single Cell Level
title_full Microenvironmental Geometry Guides Platelet Adhesion and Spreading: A Quantitative Analysis at the Single Cell Level
title_fullStr Microenvironmental Geometry Guides Platelet Adhesion and Spreading: A Quantitative Analysis at the Single Cell Level
title_full_unstemmed Microenvironmental Geometry Guides Platelet Adhesion and Spreading: A Quantitative Analysis at the Single Cell Level
title_short Microenvironmental Geometry Guides Platelet Adhesion and Spreading: A Quantitative Analysis at the Single Cell Level
title_sort microenvironmental geometry guides platelet adhesion and spreading: a quantitative analysis at the single cell level
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3197646/
https://www.ncbi.nlm.nih.gov/pubmed/22028878
http://dx.doi.org/10.1371/journal.pone.0026437
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