Optimized Generation of Functional Neutrophils and Macrophages from Patient-Specific Induced Pluripotent Stem Cells: Ex Vivo Models of X(0)-Linked, AR22(0)- and AR47(0)- Chronic Granulomatous Diseases

Chronic granulomatous disease (CGD) is an inherited orphan disorder caused by mutations in one of the five genes encoding reduced nicotinamide-adenine-dinucleotide-phosphate oxidase subunits, which subsequently lead to impairment in the production of microbicidal reactive oxygen species (ROS). In or...

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Autores principales: Brault, Julie, Goutagny, Erwan, Telugu, Narasimha, Shao, Kaifeng, Baquié, Mathurin, Satre, Véronique, Coutton, Charles, Grunwald, Didier, Brion, Jean-Paul, Barlogis, Vincent, Stephan, Jean-Louis, Plantaz, Dominique, Hescheler, Jürgen, Krause, Karl-Heinz, Šarić, Tomo, Stasia, Marie José
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Mary Ann Liebert, Inc. 2014
Materias:
Original Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4245876/
https://www.ncbi.nlm.nih.gov/pubmed/25469316
http://dx.doi.org/10.1089/biores.2014.0045
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author Brault, Julie
Goutagny, Erwan
Telugu, Narasimha
Shao, Kaifeng
Baquié, Mathurin
Satre, Véronique
Coutton, Charles
Grunwald, Didier
Brion, Jean-Paul
Barlogis, Vincent
Stephan, Jean-Louis
Plantaz, Dominique
Hescheler, Jürgen
Krause, Karl-Heinz
Šarić, Tomo
Stasia, Marie José
author_facet Brault, Julie
Goutagny, Erwan
Telugu, Narasimha
Shao, Kaifeng
Baquié, Mathurin
Satre, Véronique
Coutton, Charles
Grunwald, Didier
Brion, Jean-Paul
Barlogis, Vincent
Stephan, Jean-Louis
Plantaz, Dominique
Hescheler, Jürgen
Krause, Karl-Heinz
Šarić, Tomo
Stasia, Marie José
author_sort Brault, Julie
collection PubMed
description Chronic granulomatous disease (CGD) is an inherited orphan disorder caused by mutations in one of the five genes encoding reduced nicotinamide-adenine-dinucleotide-phosphate oxidase subunits, which subsequently lead to impairment in the production of microbicidal reactive oxygen species (ROS). In order to offer several cell line models of CGD and therefore support research on pathophysiology and new therapeutic approaches, we optimized protocols to differentiate induced pluripotent stem cells (iPSCs) from wild-type, X(0)-, AR22(0)- and AR47(0)-CGD patient's fibroblasts into neutrophils and into macrophages. Aberrant genetic clones were discarded after chromosome karyotyping and array-comparative genomic hybridization analysis. All remaining iPSC lines showed human embryonic stem cell–like morphology, expressed all tested pluripotency markers and formed embryoid bodies that contained cells originating from all three primary germ layers. Furthermore, each CGD patient-specific iPSC line retained the gp91(phox), p47(phox), and p22(phox) mutations found in the corresponding patient's neutrophils. The average production of CD34(+) progenitors was of 1.5×10(6) cells after 10 days of differentiation of 10×10(6) iPSCs. They were terminally differentiated into about 3×10(5) neutrophils or into 3×10(7) macrophages. Based on morphological, phenotypical, and functional criteria both phagocyte types were mature and indistinguishable from the native human neutrophils and macrophages. However, neutrophils and macrophages derived from X(0)-, AR22(0)-, and AR47(0)-CGD patient-specific iPSC lines lacked ROS production and the corresponding mutated proteins. To simplify the phagocytes' production upon request, progenitors can be cryopreserved. In conclusion, we describe a reproducible, simple, and efficient way to generate neutrophils and macrophages from iPSCs and provide a new cellular model for the AR22(0)-CGD genetic form that has not been described before.
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spelling pubmed-42458762014-12-02 Optimized Generation of Functional Neutrophils and Macrophages from Patient-Specific Induced Pluripotent Stem Cells: Ex Vivo Models of X(0)-Linked, AR22(0)- and AR47(0)- Chronic Granulomatous Diseases Brault, Julie Goutagny, Erwan Telugu, Narasimha Shao, Kaifeng Baquié, Mathurin Satre, Véronique Coutton, Charles Grunwald, Didier Brion, Jean-Paul Barlogis, Vincent Stephan, Jean-Louis Plantaz, Dominique Hescheler, Jürgen Krause, Karl-Heinz Šarić, Tomo Stasia, Marie José Biores Open Access Original Research Articles Chronic granulomatous disease (CGD) is an inherited orphan disorder caused by mutations in one of the five genes encoding reduced nicotinamide-adenine-dinucleotide-phosphate oxidase subunits, which subsequently lead to impairment in the production of microbicidal reactive oxygen species (ROS). In order to offer several cell line models of CGD and therefore support research on pathophysiology and new therapeutic approaches, we optimized protocols to differentiate induced pluripotent stem cells (iPSCs) from wild-type, X(0)-, AR22(0)- and AR47(0)-CGD patient's fibroblasts into neutrophils and into macrophages. Aberrant genetic clones were discarded after chromosome karyotyping and array-comparative genomic hybridization analysis. All remaining iPSC lines showed human embryonic stem cell–like morphology, expressed all tested pluripotency markers and formed embryoid bodies that contained cells originating from all three primary germ layers. Furthermore, each CGD patient-specific iPSC line retained the gp91(phox), p47(phox), and p22(phox) mutations found in the corresponding patient's neutrophils. The average production of CD34(+) progenitors was of 1.5×10(6) cells after 10 days of differentiation of 10×10(6) iPSCs. They were terminally differentiated into about 3×10(5) neutrophils or into 3×10(7) macrophages. Based on morphological, phenotypical, and functional criteria both phagocyte types were mature and indistinguishable from the native human neutrophils and macrophages. However, neutrophils and macrophages derived from X(0)-, AR22(0)-, and AR47(0)-CGD patient-specific iPSC lines lacked ROS production and the corresponding mutated proteins. To simplify the phagocytes' production upon request, progenitors can be cryopreserved. In conclusion, we describe a reproducible, simple, and efficient way to generate neutrophils and macrophages from iPSCs and provide a new cellular model for the AR22(0)-CGD genetic form that has not been described before. Mary Ann Liebert, Inc. 2014-12-01 /pmc/articles/PMC4245876/ /pubmed/25469316 http://dx.doi.org/10.1089/biores.2014.0045 Text en Copyright 2014, Mary Ann Liebert, Inc.
spellingShingle Original Research Articles
Brault, Julie
Goutagny, Erwan
Telugu, Narasimha
Shao, Kaifeng
Baquié, Mathurin
Satre, Véronique
Coutton, Charles
Grunwald, Didier
Brion, Jean-Paul
Barlogis, Vincent
Stephan, Jean-Louis
Plantaz, Dominique
Hescheler, Jürgen
Krause, Karl-Heinz
Šarić, Tomo
Stasia, Marie José
Optimized Generation of Functional Neutrophils and Macrophages from Patient-Specific Induced Pluripotent Stem Cells: Ex Vivo Models of X(0)-Linked, AR22(0)- and AR47(0)- Chronic Granulomatous Diseases
title Optimized Generation of Functional Neutrophils and Macrophages from Patient-Specific Induced Pluripotent Stem Cells: Ex Vivo Models of X(0)-Linked, AR22(0)- and AR47(0)- Chronic Granulomatous Diseases
title_full Optimized Generation of Functional Neutrophils and Macrophages from Patient-Specific Induced Pluripotent Stem Cells: Ex Vivo Models of X(0)-Linked, AR22(0)- and AR47(0)- Chronic Granulomatous Diseases
title_fullStr Optimized Generation of Functional Neutrophils and Macrophages from Patient-Specific Induced Pluripotent Stem Cells: Ex Vivo Models of X(0)-Linked, AR22(0)- and AR47(0)- Chronic Granulomatous Diseases
title_full_unstemmed Optimized Generation of Functional Neutrophils and Macrophages from Patient-Specific Induced Pluripotent Stem Cells: Ex Vivo Models of X(0)-Linked, AR22(0)- and AR47(0)- Chronic Granulomatous Diseases
title_short Optimized Generation of Functional Neutrophils and Macrophages from Patient-Specific Induced Pluripotent Stem Cells: Ex Vivo Models of X(0)-Linked, AR22(0)- and AR47(0)- Chronic Granulomatous Diseases
title_sort optimized generation of functional neutrophils and macrophages from patient-specific induced pluripotent stem cells: ex vivo models of x(0)-linked, ar22(0)- and ar47(0)- chronic granulomatous diseases
topic Original Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4245876/
https://www.ncbi.nlm.nih.gov/pubmed/25469316
http://dx.doi.org/10.1089/biores.2014.0045
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