Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator
| dc.contributor.author | Wu, Xun | |
| dc.contributor.author | Wu, Jiandong | |
| dc.contributor.author | Li, Hongzhao | |
| dc.contributor.author | Legler, Daniel F. | |
| dc.contributor.author | Marshall, Aaron J. | |
| dc.contributor.author | Lin, Francis | |
| dc.date.accessioned | 2015-08-06T10:52:56Z | |
| dc.date.available | 2015-08-06T10:52:56Z | |
| dc.date.issued | 2015 | eng |
| dc.description.abstract | T lymphocyte migration is crucial for adaptive immunity. Manipulation of signaling molecules controlling cell migration combined with in-vitro cell migration analysis provides a powerful research approach. Microfluidic devices, which can precisely configure chemoattractant gradients and allow quantitative single cell analysis, have been increasingly applied to cell migration and chemotaxis studies. However, there are a very limited number of published studies involving microfluidic migration analysis of genetically manipulated immune cells. In this study, we describe a simple microfluidic method for quantitative analysis of T cells expressing transfected chemokine receptors and other cell migration signaling probes. Using this method, we demonstrated chemotaxis of Jurkat transfectants expressing wild-type or C-terminus mutated CCR7 within a gradient of chemokine CCL19, and characterized the difference in transfectant migration mediated by wild-type and mutant CCR7. The EGFP-tagged CCR7 allows identification of CCR7-expressing transfectants in cell migration analysis and microscopy assessment of CCR7 dynamics. Collectively, our study demonstrated the effective use of the microfluidic method for studying CCR7 mediated T cell transfectant migration. We envision this developed method will provide a useful platform to functionally test various signaling mechanisms at the cell migration level. | eng |
| dc.description.version | published | |
| dc.identifier.doi | 10.1016/j.jim.2015.02.008 | eng |
| dc.identifier.pmid | 25733353 | eng |
| dc.identifier.ppn | 485137666 | |
| dc.identifier.uri | http://kops.uni-konstanz.de/handle/123456789/31535 | |
| dc.language.iso | eng | eng |
| dc.rights | terms-of-use | |
| dc.rights.uri | https://rightsstatements.org/page/InC/1.0/ | |
| dc.subject.ddc | 570 | eng |
| dc.title | Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator | eng |
| dc.type | JOURNAL_ARTICLE | eng |
| dspace.entity.type | Publication | |
| kops.citation.bibtex | @article{Wu2015Analy-31535,
year={2015},
doi={10.1016/j.jim.2015.02.008},
title={Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator},
volume={419},
issn={0022-1759},
journal={Journal of Immunological Methods},
pages={9--17},
author={Wu, Xun and Wu, Jiandong and Li, Hongzhao and Legler, Daniel F. and Marshall, Aaron J. and Lin, Francis}
} | |
| kops.citation.iso690 | WU, Xun, Jiandong WU, Hongzhao LI, Daniel F. LEGLER, Aaron J. MARSHALL, Francis LIN, 2015. Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator. In: Journal of Immunological Methods. 2015, 419, pp. 9-17. ISSN 0022-1759. eISSN 1872-7905. Available under: doi: 10.1016/j.jim.2015.02.008 | deu |
| kops.citation.iso690 | WU, Xun, Jiandong WU, Hongzhao LI, Daniel F. LEGLER, Aaron J. MARSHALL, Francis LIN, 2015. Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator. In: Journal of Immunological Methods. 2015, 419, pp. 9-17. ISSN 0022-1759. eISSN 1872-7905. Available under: doi: 10.1016/j.jim.2015.02.008 | eng |
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<dcterms:abstract xml:lang="eng">T lymphocyte migration is crucial for adaptive immunity. Manipulation of signaling molecules controlling cell migration combined with in-vitro cell migration analysis provides a powerful research approach. Microfluidic devices, which can precisely configure chemoattractant gradients and allow quantitative single cell analysis, have been increasingly applied to cell migration and chemotaxis studies. However, there are a very limited number of published studies involving microfluidic migration analysis of genetically manipulated immune cells. In this study, we describe a simple microfluidic method for quantitative analysis of T cells expressing transfected chemokine receptors and other cell migration signaling probes. Using this method, we demonstrated chemotaxis of Jurkat transfectants expressing wild-type or C-terminus mutated CCR7 within a gradient of chemokine CCL19, and characterized the difference in transfectant migration mediated by wild-type and mutant CCR7. The EGFP-tagged CCR7 allows identification of CCR7-expressing transfectants in cell migration analysis and microscopy assessment of CCR7 dynamics. Collectively, our study demonstrated the effective use of the microfluidic method for studying CCR7 mediated T cell transfectant migration. We envision this developed method will provide a useful platform to functionally test various signaling mechanisms at the cell migration level.</dcterms:abstract>
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| kops.description.openAccess | openaccessgreen | |
| kops.identifier.nbn | urn:nbn:de:bsz:352-0-291317 | |
| kops.sourcefield | Journal of Immunological Methods. 2015, <b>419</b>, pp. 9-17. ISSN 0022-1759. eISSN 1872-7905. Available under: doi: 10.1016/j.jim.2015.02.008 | deu |
| kops.sourcefield.plain | Journal of Immunological Methods. 2015, 419, pp. 9-17. ISSN 0022-1759. eISSN 1872-7905. Available under: doi: 10.1016/j.jim.2015.02.008 | deu |
| kops.sourcefield.plain | Journal of Immunological Methods. 2015, 419, pp. 9-17. ISSN 0022-1759. eISSN 1872-7905. Available under: doi: 10.1016/j.jim.2015.02.008 | eng |
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| source.bibliographicInfo.fromPage | 9 | eng |
| source.bibliographicInfo.toPage | 17 | eng |
| source.bibliographicInfo.volume | 419 | eng |
| source.identifier.eissn | 1872-7905 | eng |
| source.identifier.issn | 0022-1759 | eng |
| source.periodicalTitle | Journal of Immunological Methods | eng |
| temp.internal.duplicates | <p>Keine Dubletten gefunden. Letzte Überprüfung: 26.05.2015 11:04:52</p> | deu |
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