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Versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung

Complexity of lung microenvironment and changes in cellular composition during disease make it exceptionally hard to understand molecular mechanisms driving development of chronic lung diseases. Although recent advances in cell type–resolved approaches hold great promise for studying complex disease...

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Autores principales: Llamazares-Prada, Maria, Espinet, Elisa, Mijošek, Vedrana, Schwartz, Uwe, Lutsik, Pavlo, Tamas, Raluca, Richter, Mandy, Behrendt, Annika, Pohl, Stephanie T., Benz, Naja P., Muley, Thomas, Warth, Arne, Heußel, Claus Peter, Winter, Hauke, Landry, Jonathan J. M., Herth, Felix J.F., Mertens, Tinne C.J., Karmouty-Quintana, Harry, Koch, Ina, Benes, Vladimir, Korbel, Jan O., Waszak, Sebastian M., Trumpp, Andreas, Wyatt, David M., Stahl, Heiko F., Plass, Christoph, Jurkowska, Renata Z.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Clinical Investigation 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8026197/
https://www.ncbi.nlm.nih.gov/pubmed/33630765
http://dx.doi.org/10.1172/jci.insight.140443
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author Llamazares-Prada, Maria
Espinet, Elisa
Mijošek, Vedrana
Schwartz, Uwe
Lutsik, Pavlo
Tamas, Raluca
Richter, Mandy
Behrendt, Annika
Pohl, Stephanie T.
Benz, Naja P.
Muley, Thomas
Warth, Arne
Heußel, Claus Peter
Winter, Hauke
Landry, Jonathan J. M.
Herth, Felix J.F.
Mertens, Tinne C.J.
Karmouty-Quintana, Harry
Koch, Ina
Benes, Vladimir
Korbel, Jan O.
Waszak, Sebastian M.
Trumpp, Andreas
Wyatt, David M.
Stahl, Heiko F.
Plass, Christoph
Jurkowska, Renata Z.
author_facet Llamazares-Prada, Maria
Espinet, Elisa
Mijošek, Vedrana
Schwartz, Uwe
Lutsik, Pavlo
Tamas, Raluca
Richter, Mandy
Behrendt, Annika
Pohl, Stephanie T.
Benz, Naja P.
Muley, Thomas
Warth, Arne
Heußel, Claus Peter
Winter, Hauke
Landry, Jonathan J. M.
Herth, Felix J.F.
Mertens, Tinne C.J.
Karmouty-Quintana, Harry
Koch, Ina
Benes, Vladimir
Korbel, Jan O.
Waszak, Sebastian M.
Trumpp, Andreas
Wyatt, David M.
Stahl, Heiko F.
Plass, Christoph
Jurkowska, Renata Z.
author_sort Llamazares-Prada, Maria
collection PubMed
description Complexity of lung microenvironment and changes in cellular composition during disease make it exceptionally hard to understand molecular mechanisms driving development of chronic lung diseases. Although recent advances in cell type–resolved approaches hold great promise for studying complex diseases, their implementation relies on local access to fresh tissue, as traditional tissue storage methods do not allow viable cell isolation. To overcome these hurdles, we developed a versatile workflow that allows storage of lung tissue with high viability, permits thorough sample quality check before cell isolation, and befits sequencing-based profiling. We demonstrate that cryopreservation enables isolation of multiple cell types from both healthy and diseased lungs. Basal cells from cryopreserved airways retain their differentiation ability, indicating that cellular identity is not altered by cryopreservation. Importantly, using RNA sequencing and EPIC Array, we show that gene expression and DNA methylation signatures are preserved upon cryopreservation, emphasizing the suitability of our workflow for omics profiling of lung cells. Moreover, we obtained high-quality single-cell RNA-sequencing data of cells from cryopreserved human lungs, demonstrating that cryopreservation empowers single-cell approaches. Overall, thanks to its simplicity, our workflow is well suited for prospective tissue collection by academic collaborators and biobanks, opening worldwide access to viable human tissue.
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spelling pubmed-80261972021-04-13 Versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung Llamazares-Prada, Maria Espinet, Elisa Mijošek, Vedrana Schwartz, Uwe Lutsik, Pavlo Tamas, Raluca Richter, Mandy Behrendt, Annika Pohl, Stephanie T. Benz, Naja P. Muley, Thomas Warth, Arne Heußel, Claus Peter Winter, Hauke Landry, Jonathan J. M. Herth, Felix J.F. Mertens, Tinne C.J. Karmouty-Quintana, Harry Koch, Ina Benes, Vladimir Korbel, Jan O. Waszak, Sebastian M. Trumpp, Andreas Wyatt, David M. Stahl, Heiko F. Plass, Christoph Jurkowska, Renata Z. JCI Insight Technical Advance Complexity of lung microenvironment and changes in cellular composition during disease make it exceptionally hard to understand molecular mechanisms driving development of chronic lung diseases. Although recent advances in cell type–resolved approaches hold great promise for studying complex diseases, their implementation relies on local access to fresh tissue, as traditional tissue storage methods do not allow viable cell isolation. To overcome these hurdles, we developed a versatile workflow that allows storage of lung tissue with high viability, permits thorough sample quality check before cell isolation, and befits sequencing-based profiling. We demonstrate that cryopreservation enables isolation of multiple cell types from both healthy and diseased lungs. Basal cells from cryopreserved airways retain their differentiation ability, indicating that cellular identity is not altered by cryopreservation. Importantly, using RNA sequencing and EPIC Array, we show that gene expression and DNA methylation signatures are preserved upon cryopreservation, emphasizing the suitability of our workflow for omics profiling of lung cells. Moreover, we obtained high-quality single-cell RNA-sequencing data of cells from cryopreserved human lungs, demonstrating that cryopreservation empowers single-cell approaches. Overall, thanks to its simplicity, our workflow is well suited for prospective tissue collection by academic collaborators and biobanks, opening worldwide access to viable human tissue. American Society for Clinical Investigation 2021-03-22 /pmc/articles/PMC8026197/ /pubmed/33630765 http://dx.doi.org/10.1172/jci.insight.140443 Text en © 2021 Llamazares-Prada et al. https://creativecommons.org/licenses/by/4.0/This work is licensed under the Creative Commons Attribution 4.0 International License. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Technical Advance
Llamazares-Prada, Maria
Espinet, Elisa
Mijošek, Vedrana
Schwartz, Uwe
Lutsik, Pavlo
Tamas, Raluca
Richter, Mandy
Behrendt, Annika
Pohl, Stephanie T.
Benz, Naja P.
Muley, Thomas
Warth, Arne
Heußel, Claus Peter
Winter, Hauke
Landry, Jonathan J. M.
Herth, Felix J.F.
Mertens, Tinne C.J.
Karmouty-Quintana, Harry
Koch, Ina
Benes, Vladimir
Korbel, Jan O.
Waszak, Sebastian M.
Trumpp, Andreas
Wyatt, David M.
Stahl, Heiko F.
Plass, Christoph
Jurkowska, Renata Z.
Versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung
title Versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung
title_full Versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung
title_fullStr Versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung
title_full_unstemmed Versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung
title_short Versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung
title_sort versatile workflow for cell type–resolved transcriptional and epigenetic profiles from cryopreserved human lung
topic Technical Advance
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8026197/
https://www.ncbi.nlm.nih.gov/pubmed/33630765
http://dx.doi.org/10.1172/jci.insight.140443
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