Orchestration of human multi‐lineage hematopoietic cell development by humanized in vivo bone marrow models
Abstract Hematopoiesis develops in the bone marrow (BM) where multiple interactions regulate the differentiation and preservation of hematopoietic stem and progenitor cells (HSPCs). Immune‐deficient murine models have enabled the analysis of molecular and cellular regulation of human HSPCs, but the...
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Wiley
2025-04-01
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| Online Access: | https://doi.org/10.1002/hem3.70120 |
| _version_ | 1848763477386067968 |
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| author | Laurent Renou Wenjie Sun Chloe Friedrich Klaudia Galant Cecile Conrad Anne Consalus Evelia Plantier Katharina Schallmoser Linda Krisch Vilma Barroca Saryami Devanand Nathalie Dechamps Andreas Reinisch Jelena Martinovic Alessandra Magnani Lionel Faivre Daniel Lewandowski Julien Calvo Leila Perie Olivier Kosmider Françoise Pflumio |
| author_facet | Laurent Renou Wenjie Sun Chloe Friedrich Klaudia Galant Cecile Conrad Anne Consalus Evelia Plantier Katharina Schallmoser Linda Krisch Vilma Barroca Saryami Devanand Nathalie Dechamps Andreas Reinisch Jelena Martinovic Alessandra Magnani Lionel Faivre Daniel Lewandowski Julien Calvo Leila Perie Olivier Kosmider Françoise Pflumio |
| author_sort | Laurent Renou |
| collection | DOAJ |
| container_title | HemaSphere |
| description | Abstract Hematopoiesis develops in the bone marrow (BM) where multiple interactions regulate the differentiation and preservation of hematopoietic stem and progenitor cells (HSPCs). Immune‐deficient murine models have enabled the analysis of molecular and cellular regulation of human HSPCs, but the physiology of these models is questioned as human hematopoietic cells develop in xenogenic microenvironments. In this study, we thoroughly characterized a humanized (h) in vivo BM model, developed from fetal (F/) and post‐natal (P‐N/) mesenchymal stromal cell (MSC) differentiation (called hOssicles [hOss]), in which human hematopoietic cells are generated following the transplantation of CD34+ cells. Serial isolation and transplant experiments of hMSCs and HSPCs from hOss revealed the dynamic nature of these hBM niches. hOss modified human hematopoietic development by modulating myeloid/lymphoid cell production and HSPC levels, with no major transcriptional changes in HSPCs at the single‐cell level. Clonal tracking using genetic barcodes highlighted hematopoietic cell cross‐talks between the endogenous murine BM and hOss and differences in clonal myeloid/multipotent cell production between F/hOss and P‐N/hOss, uncovering ontogeny‐related impact of the BM on human hematopoietic cell production. |
| format | Article |
| id | doaj-art-e9c2ef7756b847e8b0fb6c8d5787e17a |
| institution | Directory of Open Access Journals |
| issn | 2572-9241 |
| language | English |
| publishDate | 2025-04-01 |
| publisher | Wiley |
| record_format | Article |
| spelling | doaj-art-e9c2ef7756b847e8b0fb6c8d5787e17a2025-10-08T10:39:30ZengWileyHemaSphere2572-92412025-04-0194n/an/a10.1002/hem3.70120Orchestration of human multi‐lineage hematopoietic cell development by humanized in vivo bone marrow modelsLaurent Renou0Wenjie Sun1Chloe Friedrich2Klaudia Galant3Cecile Conrad4Anne Consalus5Evelia Plantier6Katharina Schallmoser7Linda Krisch8Vilma Barroca9Saryami Devanand10Nathalie Dechamps11Andreas Reinisch12Jelena Martinovic13Alessandra Magnani14Lionel Faivre15Daniel Lewandowski16Julien Calvo17Leila Perie18Olivier Kosmider19Françoise Pflumio20Université Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceInstitut Curie, Université PSL, Sorbonne Université, CNRS UMR168, Laboratoire Physico Chimie Curie Paris FranceInstitut Cochin, CNRS UMR8104, INSERM U1016 Université Paris Cité Paris FranceUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceInstitut Curie, Université PSL, Sorbonne Université, CNRS UMR168, Laboratoire Physico Chimie Curie Paris FranceUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceDepartment for Transfusion Medicine and GMP Unit Paracelsus Medical University Salzburg AustriaDepartment for Transfusion Medicine and GMP Unit Paracelsus Medical University Salzburg AustriaUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceDepartment of Internal Medicine, Division of Hematology Medical University of Graz Graz AustriaFetal Pathology Unit AP‐HP, Hôpital Antoine Beclère Clamart FranceBiotherapy Department Hôpital Necker‐Enfants Malades Paris FranceCell Therapy Unit AP‐HP, Saint Louis Hospital Paris FranceUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceInstitut Curie, Université PSL, Sorbonne Université, CNRS UMR168, Laboratoire Physico Chimie Curie Paris FranceOPALE Carnot Institute, The Organization for Partnerships in Leukemia Paris FranceUniversité Paris Cité, Inserm, CEA, Stabilité Génétique Cellules Souches et Radiations, LSHL/iRCM/IBFJ Fontenay‐aux‐Roses FranceAbstract Hematopoiesis develops in the bone marrow (BM) where multiple interactions regulate the differentiation and preservation of hematopoietic stem and progenitor cells (HSPCs). Immune‐deficient murine models have enabled the analysis of molecular and cellular regulation of human HSPCs, but the physiology of these models is questioned as human hematopoietic cells develop in xenogenic microenvironments. In this study, we thoroughly characterized a humanized (h) in vivo BM model, developed from fetal (F/) and post‐natal (P‐N/) mesenchymal stromal cell (MSC) differentiation (called hOssicles [hOss]), in which human hematopoietic cells are generated following the transplantation of CD34+ cells. Serial isolation and transplant experiments of hMSCs and HSPCs from hOss revealed the dynamic nature of these hBM niches. hOss modified human hematopoietic development by modulating myeloid/lymphoid cell production and HSPC levels, with no major transcriptional changes in HSPCs at the single‐cell level. Clonal tracking using genetic barcodes highlighted hematopoietic cell cross‐talks between the endogenous murine BM and hOss and differences in clonal myeloid/multipotent cell production between F/hOss and P‐N/hOss, uncovering ontogeny‐related impact of the BM on human hematopoietic cell production.https://doi.org/10.1002/hem3.70120 |
| spellingShingle | Laurent Renou Wenjie Sun Chloe Friedrich Klaudia Galant Cecile Conrad Anne Consalus Evelia Plantier Katharina Schallmoser Linda Krisch Vilma Barroca Saryami Devanand Nathalie Dechamps Andreas Reinisch Jelena Martinovic Alessandra Magnani Lionel Faivre Daniel Lewandowski Julien Calvo Leila Perie Olivier Kosmider Françoise Pflumio Orchestration of human multi‐lineage hematopoietic cell development by humanized in vivo bone marrow models |
| title | Orchestration of human multi‐lineage hematopoietic cell development by humanized in vivo bone marrow models |
| title_full | Orchestration of human multi‐lineage hematopoietic cell development by humanized in vivo bone marrow models |
| title_fullStr | Orchestration of human multi‐lineage hematopoietic cell development by humanized in vivo bone marrow models |
| title_full_unstemmed | Orchestration of human multi‐lineage hematopoietic cell development by humanized in vivo bone marrow models |
| title_short | Orchestration of human multi‐lineage hematopoietic cell development by humanized in vivo bone marrow models |
| title_sort | orchestration of human multi lineage hematopoietic cell development by humanized in vivo bone marrow models |
| url | https://doi.org/10.1002/hem3.70120 |
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