A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases

BACKGROUND: Genomic medicine has paved the way for identifying biomarkers and therapeutically actionable targets for complex diseases, but is complicated by the involvement of thousands of variably expressed genes across multiple cell types. Single-cell RNA-sequencing study (scRNA-seq) allows the ch...

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Autores principales: Gawel, Danuta R., Serra-Musach, Jordi, Lilja, Sandra, Aagesen, Jesper, Arenas, Alex, Asking, Bengt, Bengnér, Malin, Björkander, Janne, Biggs, Sophie, Ernerudh, Jan, Hjortswang, Henrik, Karlsson, Jan-Erik, Köpsen, Mattias, Lee, Eun Jung, Lentini, Antonio, Li, Xinxiu, Magnusson, Mattias, Martínez-Enguita, David, Matussek, Andreas, Nestor, Colm E., Schäfer, Samuel, Seifert, Oliver, Sonmez, Ceylan, Stjernman, Henrik, Tjärnberg, Andreas, Wu, Simon, Åkesson, Karin, Shalek, Alex K., Stenmarker, Margaretha, Zhang, Huan, Gustafsson, Mika, Benson, Mikael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2019
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6664760/
https://www.ncbi.nlm.nih.gov/pubmed/31358043
http://dx.doi.org/10.1186/s13073-019-0657-3
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author Gawel, Danuta R.
Serra-Musach, Jordi
Lilja, Sandra
Aagesen, Jesper
Arenas, Alex
Asking, Bengt
Bengnér, Malin
Björkander, Janne
Biggs, Sophie
Ernerudh, Jan
Hjortswang, Henrik
Karlsson, Jan-Erik
Köpsen, Mattias
Lee, Eun Jung
Lentini, Antonio
Li, Xinxiu
Magnusson, Mattias
Martínez-Enguita, David
Matussek, Andreas
Nestor, Colm E.
Schäfer, Samuel
Seifert, Oliver
Sonmez, Ceylan
Stjernman, Henrik
Tjärnberg, Andreas
Wu, Simon
Åkesson, Karin
Shalek, Alex K.
Stenmarker, Margaretha
Zhang, Huan
Gustafsson, Mika
Benson, Mikael
author_facet Gawel, Danuta R.
Serra-Musach, Jordi
Lilja, Sandra
Aagesen, Jesper
Arenas, Alex
Asking, Bengt
Bengnér, Malin
Björkander, Janne
Biggs, Sophie
Ernerudh, Jan
Hjortswang, Henrik
Karlsson, Jan-Erik
Köpsen, Mattias
Lee, Eun Jung
Lentini, Antonio
Li, Xinxiu
Magnusson, Mattias
Martínez-Enguita, David
Matussek, Andreas
Nestor, Colm E.
Schäfer, Samuel
Seifert, Oliver
Sonmez, Ceylan
Stjernman, Henrik
Tjärnberg, Andreas
Wu, Simon
Åkesson, Karin
Shalek, Alex K.
Stenmarker, Margaretha
Zhang, Huan
Gustafsson, Mika
Benson, Mikael
author_sort Gawel, Danuta R.
collection PubMed
description BACKGROUND: Genomic medicine has paved the way for identifying biomarkers and therapeutically actionable targets for complex diseases, but is complicated by the involvement of thousands of variably expressed genes across multiple cell types. Single-cell RNA-sequencing study (scRNA-seq) allows the characterization of such complex changes in whole organs. METHODS: The study is based on applying network tools to organize and analyze scRNA-seq data from a mouse model of arthritis and human rheumatoid arthritis, in order to find diagnostic biomarkers and therapeutic targets. Diagnostic validation studies were performed using expression profiling data and potential protein biomarkers from prospective clinical studies of 13 diseases. A candidate drug was examined by a treatment study of a mouse model of arthritis, using phenotypic, immunohistochemical, and cellular analyses as read-outs. RESULTS: We performed the first systematic analysis of pathways, potential biomarkers, and drug targets in scRNA-seq data from a complex disease, starting with inflamed joints and lymph nodes from a mouse model of arthritis. We found the involvement of hundreds of pathways, biomarkers, and drug targets that differed greatly between cell types. Analyses of scRNA-seq and GWAS data from human rheumatoid arthritis (RA) supported a similar dispersion of pathogenic mechanisms in different cell types. Thus, systems-level approaches to prioritize biomarkers and drugs are needed. Here, we present a prioritization strategy that is based on constructing network models of disease-associated cell types and interactions using scRNA-seq data from our mouse model of arthritis, as well as human RA, which we term multicellular disease models (MCDMs). We find that the network centrality of MCDM cell types correlates with the enrichment of genes harboring genetic variants associated with RA and thus could potentially be used to prioritize cell types and genes for diagnostics and therapeutics. We validated this hypothesis in a large-scale study of patients with 13 different autoimmune, allergic, infectious, malignant, endocrine, metabolic, and cardiovascular diseases, as well as a therapeutic study of the mouse arthritis model. CONCLUSIONS: Overall, our results support that our strategy has the potential to help prioritize diagnostic and therapeutic targets in human disease. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s13073-019-0657-3) contains supplementary material, which is available to authorized users.
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spelling pubmed-66647602019-08-05 A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases Gawel, Danuta R. Serra-Musach, Jordi Lilja, Sandra Aagesen, Jesper Arenas, Alex Asking, Bengt Bengnér, Malin Björkander, Janne Biggs, Sophie Ernerudh, Jan Hjortswang, Henrik Karlsson, Jan-Erik Köpsen, Mattias Lee, Eun Jung Lentini, Antonio Li, Xinxiu Magnusson, Mattias Martínez-Enguita, David Matussek, Andreas Nestor, Colm E. Schäfer, Samuel Seifert, Oliver Sonmez, Ceylan Stjernman, Henrik Tjärnberg, Andreas Wu, Simon Åkesson, Karin Shalek, Alex K. Stenmarker, Margaretha Zhang, Huan Gustafsson, Mika Benson, Mikael Genome Med Research BACKGROUND: Genomic medicine has paved the way for identifying biomarkers and therapeutically actionable targets for complex diseases, but is complicated by the involvement of thousands of variably expressed genes across multiple cell types. Single-cell RNA-sequencing study (scRNA-seq) allows the characterization of such complex changes in whole organs. METHODS: The study is based on applying network tools to organize and analyze scRNA-seq data from a mouse model of arthritis and human rheumatoid arthritis, in order to find diagnostic biomarkers and therapeutic targets. Diagnostic validation studies were performed using expression profiling data and potential protein biomarkers from prospective clinical studies of 13 diseases. A candidate drug was examined by a treatment study of a mouse model of arthritis, using phenotypic, immunohistochemical, and cellular analyses as read-outs. RESULTS: We performed the first systematic analysis of pathways, potential biomarkers, and drug targets in scRNA-seq data from a complex disease, starting with inflamed joints and lymph nodes from a mouse model of arthritis. We found the involvement of hundreds of pathways, biomarkers, and drug targets that differed greatly between cell types. Analyses of scRNA-seq and GWAS data from human rheumatoid arthritis (RA) supported a similar dispersion of pathogenic mechanisms in different cell types. Thus, systems-level approaches to prioritize biomarkers and drugs are needed. Here, we present a prioritization strategy that is based on constructing network models of disease-associated cell types and interactions using scRNA-seq data from our mouse model of arthritis, as well as human RA, which we term multicellular disease models (MCDMs). We find that the network centrality of MCDM cell types correlates with the enrichment of genes harboring genetic variants associated with RA and thus could potentially be used to prioritize cell types and genes for diagnostics and therapeutics. We validated this hypothesis in a large-scale study of patients with 13 different autoimmune, allergic, infectious, malignant, endocrine, metabolic, and cardiovascular diseases, as well as a therapeutic study of the mouse arthritis model. CONCLUSIONS: Overall, our results support that our strategy has the potential to help prioritize diagnostic and therapeutic targets in human disease. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s13073-019-0657-3) contains supplementary material, which is available to authorized users. BioMed Central 2019-07-30 /pmc/articles/PMC6664760/ /pubmed/31358043 http://dx.doi.org/10.1186/s13073-019-0657-3 Text en © The Author(s). 2019 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Gawel, Danuta R.
Serra-Musach, Jordi
Lilja, Sandra
Aagesen, Jesper
Arenas, Alex
Asking, Bengt
Bengnér, Malin
Björkander, Janne
Biggs, Sophie
Ernerudh, Jan
Hjortswang, Henrik
Karlsson, Jan-Erik
Köpsen, Mattias
Lee, Eun Jung
Lentini, Antonio
Li, Xinxiu
Magnusson, Mattias
Martínez-Enguita, David
Matussek, Andreas
Nestor, Colm E.
Schäfer, Samuel
Seifert, Oliver
Sonmez, Ceylan
Stjernman, Henrik
Tjärnberg, Andreas
Wu, Simon
Åkesson, Karin
Shalek, Alex K.
Stenmarker, Margaretha
Zhang, Huan
Gustafsson, Mika
Benson, Mikael
A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases
title A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases
title_full A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases
title_fullStr A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases
title_full_unstemmed A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases
title_short A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases
title_sort validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6664760/
https://www.ncbi.nlm.nih.gov/pubmed/31358043
http://dx.doi.org/10.1186/s13073-019-0657-3
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