Pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of M2-like macrophages

Human Mesenchymal Stromal Cells (hMSCs) are a promising source for cell-based therapies. Yet, transition to phase III and IV clinical trials is remarkably slow. To mitigate donor variabilities and to obtain robust and valid clinical data, we aimed first to develop a manufacturing concept balancing l...

Descripción completa

Detalles Bibliográficos
Autores principales: Willer, Hélène, Spohn, Gabriele, Morgenroth, Kimberly, Thielemann, Corinna, Elvers-Hornung, Susanne, Bugert, Peter, Delorme, Bruno, Giesen, Melanie, Schmitz-Rixen, Thomas, Seifried, Erhard, Pfarrer, Christiane, Schäfer, Richard, Bieback, Karen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9437960/
https://www.ncbi.nlm.nih.gov/pubmed/36059533
http://dx.doi.org/10.3389/fimmu.2022.976511
_version_ 1784781725831790592
author Willer, Hélène
Spohn, Gabriele
Morgenroth, Kimberly
Thielemann, Corinna
Elvers-Hornung, Susanne
Bugert, Peter
Delorme, Bruno
Giesen, Melanie
Schmitz-Rixen, Thomas
Seifried, Erhard
Pfarrer, Christiane
Schäfer, Richard
Bieback, Karen
author_facet Willer, Hélène
Spohn, Gabriele
Morgenroth, Kimberly
Thielemann, Corinna
Elvers-Hornung, Susanne
Bugert, Peter
Delorme, Bruno
Giesen, Melanie
Schmitz-Rixen, Thomas
Seifried, Erhard
Pfarrer, Christiane
Schäfer, Richard
Bieback, Karen
author_sort Willer, Hélène
collection PubMed
description Human Mesenchymal Stromal Cells (hMSCs) are a promising source for cell-based therapies. Yet, transition to phase III and IV clinical trials is remarkably slow. To mitigate donor variabilities and to obtain robust and valid clinical data, we aimed first to develop a manufacturing concept balancing large-scale production of pooled hMSCs in a minimal expansion period, and second to test them for key manufacture and efficacy indicators in the clinically highly relevant indication wound healing. Our novel clinical-scale manufacturing concept is comprised of six single donor hMSCs master cell banks that are pooled to a working cell bank from which an extrapolated number of 70,000 clinical doses of 1x10(6) hMSCs/cm(2) wound size can be manufactured within only three passages. The pooled hMSC batches showed high stability of key manufacture indicators such as morphology, immune phenotype, proliferation, scratch wound healing, chemotactic migration and angiogenic support. Repeated topical hMSCs administration significantly accelerated the wound healing in a diabetic rat model by delivering a defined growth factor cargo (specifically BDNF, EGF, G-CSF, HGF, IL-1α, IL-6, LIF, osteopontin, VEGF-A, FGF-2, TGF-β, PGE-2 and IDO after priming) at the specific stages of wound repair, namely inflammation, proliferation and remodeling. Specifically, the hMSCs mediated epidermal and dermal maturation and collagen formation, improved vascularization, and promoted cell infiltration. Kinetic analyses revealed transient presence of hMSCs until day (d)4, and the dynamic recruitment of macrophages infiltrating from the wound edges (d3) and basis (d9), eventually progressing to the apical wound on d11. In the wounds, the hMSCs mediated M2-like macrophage polarization starting at d4, peaking at d9 and then decreasing to d11. Our study establishes a standardized, scalable and pooled hMSC therapeutic, delivering a defined cargo of trophic factors, which is efficacious in diabetic wound healing by improving vascularization and dynamic recruitment of M2-like macrophages. This decision-making study now enables the validation of pooled hMSCs as treatment for impaired wound healing in large randomized clinical trials.
format Online
Article
Text
id pubmed-9437960
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-94379602022-09-03 Pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of M2-like macrophages Willer, Hélène Spohn, Gabriele Morgenroth, Kimberly Thielemann, Corinna Elvers-Hornung, Susanne Bugert, Peter Delorme, Bruno Giesen, Melanie Schmitz-Rixen, Thomas Seifried, Erhard Pfarrer, Christiane Schäfer, Richard Bieback, Karen Front Immunol Immunology Human Mesenchymal Stromal Cells (hMSCs) are a promising source for cell-based therapies. Yet, transition to phase III and IV clinical trials is remarkably slow. To mitigate donor variabilities and to obtain robust and valid clinical data, we aimed first to develop a manufacturing concept balancing large-scale production of pooled hMSCs in a minimal expansion period, and second to test them for key manufacture and efficacy indicators in the clinically highly relevant indication wound healing. Our novel clinical-scale manufacturing concept is comprised of six single donor hMSCs master cell banks that are pooled to a working cell bank from which an extrapolated number of 70,000 clinical doses of 1x10(6) hMSCs/cm(2) wound size can be manufactured within only three passages. The pooled hMSC batches showed high stability of key manufacture indicators such as morphology, immune phenotype, proliferation, scratch wound healing, chemotactic migration and angiogenic support. Repeated topical hMSCs administration significantly accelerated the wound healing in a diabetic rat model by delivering a defined growth factor cargo (specifically BDNF, EGF, G-CSF, HGF, IL-1α, IL-6, LIF, osteopontin, VEGF-A, FGF-2, TGF-β, PGE-2 and IDO after priming) at the specific stages of wound repair, namely inflammation, proliferation and remodeling. Specifically, the hMSCs mediated epidermal and dermal maturation and collagen formation, improved vascularization, and promoted cell infiltration. Kinetic analyses revealed transient presence of hMSCs until day (d)4, and the dynamic recruitment of macrophages infiltrating from the wound edges (d3) and basis (d9), eventually progressing to the apical wound on d11. In the wounds, the hMSCs mediated M2-like macrophage polarization starting at d4, peaking at d9 and then decreasing to d11. Our study establishes a standardized, scalable and pooled hMSC therapeutic, delivering a defined cargo of trophic factors, which is efficacious in diabetic wound healing by improving vascularization and dynamic recruitment of M2-like macrophages. This decision-making study now enables the validation of pooled hMSCs as treatment for impaired wound healing in large randomized clinical trials. Frontiers Media S.A. 2022-08-19 /pmc/articles/PMC9437960/ /pubmed/36059533 http://dx.doi.org/10.3389/fimmu.2022.976511 Text en Copyright © 2022 Willer, Spohn, Morgenroth, Thielemann, Elvers-Hornung, Bugert, Delorme, Giesen, Schmitz-Rixen, Seifried, Pfarrer, Schäfer and Bieback https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Willer, Hélène
Spohn, Gabriele
Morgenroth, Kimberly
Thielemann, Corinna
Elvers-Hornung, Susanne
Bugert, Peter
Delorme, Bruno
Giesen, Melanie
Schmitz-Rixen, Thomas
Seifried, Erhard
Pfarrer, Christiane
Schäfer, Richard
Bieback, Karen
Pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of M2-like macrophages
title Pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of M2-like macrophages
title_full Pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of M2-like macrophages
title_fullStr Pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of M2-like macrophages
title_full_unstemmed Pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of M2-like macrophages
title_short Pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of M2-like macrophages
title_sort pooled human bone marrow-derived mesenchymal stromal cells with defined trophic factors cargo promote dermal wound healing in diabetic rats by improved vascularization and dynamic recruitment of m2-like macrophages
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9437960/
https://www.ncbi.nlm.nih.gov/pubmed/36059533
http://dx.doi.org/10.3389/fimmu.2022.976511
work_keys_str_mv AT willerhelene pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT spohngabriele pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT morgenrothkimberly pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT thielemanncorinna pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT elvershornungsusanne pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT bugertpeter pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT delormebruno pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT giesenmelanie pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT schmitzrixenthomas pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT seifriederhard pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT pfarrerchristiane pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT schaferrichard pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages
AT biebackkaren pooledhumanbonemarrowderivedmesenchymalstromalcellswithdefinedtrophicfactorscargopromotedermalwoundhealingindiabeticratsbyimprovedvascularizationanddynamicrecruitmentofm2likemacrophages

Ejemplares similares