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The centrosomal protein 83 (CEP83) regulates human pluripotent stem cell differentiation toward the kidney lineage

During embryonic development, the mesoderm undergoes patterning into diverse lineages including axial, paraxial, and lateral plate mesoderm (LPM). Within the LPM, the so-called intermediate mesoderm (IM) forms kidney and urogenital tract progenitor cells, while the remaining LPM forms cardiovascular...

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Autores principales: Mansour, Fatma, Hinze, Christian, Telugu, Narasimha Swamy, Kresoja, Jelena, Shaheed, Iman B, Mosimann, Christian, Diecke, Sebastian, Schmidt-Ott, Kai M
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9629839/
https://www.ncbi.nlm.nih.gov/pubmed/36222666
http://dx.doi.org/10.7554/eLife.80165
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author Mansour, Fatma
Hinze, Christian
Telugu, Narasimha Swamy
Kresoja, Jelena
Shaheed, Iman B
Mosimann, Christian
Diecke, Sebastian
Schmidt-Ott, Kai M
author_facet Mansour, Fatma
Hinze, Christian
Telugu, Narasimha Swamy
Kresoja, Jelena
Shaheed, Iman B
Mosimann, Christian
Diecke, Sebastian
Schmidt-Ott, Kai M
author_sort Mansour, Fatma
collection PubMed
description During embryonic development, the mesoderm undergoes patterning into diverse lineages including axial, paraxial, and lateral plate mesoderm (LPM). Within the LPM, the so-called intermediate mesoderm (IM) forms kidney and urogenital tract progenitor cells, while the remaining LPM forms cardiovascular, hematopoietic, mesothelial, and additional progenitor cells. The signals that regulate these early lineage decisions are incompletely understood. Here, we found that the centrosomal protein 83 (CEP83), a centriolar component necessary for primary cilia formation and mutated in pediatric kidney disease, influences the differentiation of human-induced pluripotent stem cells (hiPSCs) toward IM. We induced inactivating deletions of CEP83 in hiPSCs and applied a 7-day in vitro protocol of IM kidney progenitor differentiation, based on timed application of WNT and FGF agonists. We characterized induced mesodermal cell populations using single-cell and bulk transcriptomics and tested their ability to form kidney structures in subsequent organoid culture. While hiPSCs with homozygous CEP83 inactivation were normal regarding morphology and transcriptome, their induced differentiation into IM progenitor cells was perturbed. Mesodermal cells induced after 7 days of monolayer culture of CEP83-deficient hiPCS exhibited absent or elongated primary cilia, displayed decreased expression of critical IM genes (PAX8, EYA1, HOXB7), and an aberrant induction of LPM markers (e.g. FOXF1, FOXF2, FENDRR, HAND1, HAND2). Upon subsequent organoid culture, wildtype cells differentiated to form kidney tubules and glomerular-like structures, whereas CEP83-deficient cells failed to generate kidney cell types, instead upregulating cardiomyocyte, vascular, and more general LPM progenitor markers. Our data suggest that CEP83 regulates the balance of IM and LPM formation from human pluripotent stem cells, identifying a potential link between centriolar or ciliary function and mesodermal lineage induction.
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spelling pubmed-96298392022-11-03 The centrosomal protein 83 (CEP83) regulates human pluripotent stem cell differentiation toward the kidney lineage Mansour, Fatma Hinze, Christian Telugu, Narasimha Swamy Kresoja, Jelena Shaheed, Iman B Mosimann, Christian Diecke, Sebastian Schmidt-Ott, Kai M eLife Cell Biology During embryonic development, the mesoderm undergoes patterning into diverse lineages including axial, paraxial, and lateral plate mesoderm (LPM). Within the LPM, the so-called intermediate mesoderm (IM) forms kidney and urogenital tract progenitor cells, while the remaining LPM forms cardiovascular, hematopoietic, mesothelial, and additional progenitor cells. The signals that regulate these early lineage decisions are incompletely understood. Here, we found that the centrosomal protein 83 (CEP83), a centriolar component necessary for primary cilia formation and mutated in pediatric kidney disease, influences the differentiation of human-induced pluripotent stem cells (hiPSCs) toward IM. We induced inactivating deletions of CEP83 in hiPSCs and applied a 7-day in vitro protocol of IM kidney progenitor differentiation, based on timed application of WNT and FGF agonists. We characterized induced mesodermal cell populations using single-cell and bulk transcriptomics and tested their ability to form kidney structures in subsequent organoid culture. While hiPSCs with homozygous CEP83 inactivation were normal regarding morphology and transcriptome, their induced differentiation into IM progenitor cells was perturbed. Mesodermal cells induced after 7 days of monolayer culture of CEP83-deficient hiPCS exhibited absent or elongated primary cilia, displayed decreased expression of critical IM genes (PAX8, EYA1, HOXB7), and an aberrant induction of LPM markers (e.g. FOXF1, FOXF2, FENDRR, HAND1, HAND2). Upon subsequent organoid culture, wildtype cells differentiated to form kidney tubules and glomerular-like structures, whereas CEP83-deficient cells failed to generate kidney cell types, instead upregulating cardiomyocyte, vascular, and more general LPM progenitor markers. Our data suggest that CEP83 regulates the balance of IM and LPM formation from human pluripotent stem cells, identifying a potential link between centriolar or ciliary function and mesodermal lineage induction. eLife Sciences Publications, Ltd 2022-10-12 /pmc/articles/PMC9629839/ /pubmed/36222666 http://dx.doi.org/10.7554/eLife.80165 Text en © 2022, Mansour et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Cell Biology
Mansour, Fatma
Hinze, Christian
Telugu, Narasimha Swamy
Kresoja, Jelena
Shaheed, Iman B
Mosimann, Christian
Diecke, Sebastian
Schmidt-Ott, Kai M
The centrosomal protein 83 (CEP83) regulates human pluripotent stem cell differentiation toward the kidney lineage
title The centrosomal protein 83 (CEP83) regulates human pluripotent stem cell differentiation toward the kidney lineage
title_full The centrosomal protein 83 (CEP83) regulates human pluripotent stem cell differentiation toward the kidney lineage
title_fullStr The centrosomal protein 83 (CEP83) regulates human pluripotent stem cell differentiation toward the kidney lineage
title_full_unstemmed The centrosomal protein 83 (CEP83) regulates human pluripotent stem cell differentiation toward the kidney lineage
title_short The centrosomal protein 83 (CEP83) regulates human pluripotent stem cell differentiation toward the kidney lineage
title_sort centrosomal protein 83 (cep83) regulates human pluripotent stem cell differentiation toward the kidney lineage
topic Cell Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9629839/
https://www.ncbi.nlm.nih.gov/pubmed/36222666
http://dx.doi.org/10.7554/eLife.80165
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