Human MuStem cells are competent to fuse with nonhuman primate myofibers in a clinically relevant transplantation context: A proof-of-concept study

Author:

Charrier Marine123,Leroux Isabelle1,Pichon Julien1,Schleder Cindy1,Larcher Thibaut1,Hamel Antoine4,Magot Armelle5,Péréon Yann5,Lamirault Guillaume2,Tremblay Jacques P6,Skuk Daniel6ORCID,Rouger Karl1ORCID

Affiliation:

1. Oniris, INRAE, PAnTher , Nantes, France

2. L’institut du Thorax, INSERM, CNRS, UNIV Nantes , Nantes, France

3. Nantes Université , Nantes, France

4. Service de Chirurgie Infantile, Centre Hospitalier Universitaire (CHU) de Nantes , Nantes, France

5. Centre de Référence Maladies Neuromusculaires AOC, Filnemus, Euro-NMD, Laboratoire d’Explorations Fonctionnelles, Centre Hospitalier Universitaire Hôtel Dieu , Nantes, France

6. Axe Neurosciences, Research Center of the CHU de Quebec—CHUL and Department of Molecular Medicine, School of Medicine, Laval University , Quebec, Quebec, Canada

Abstract

Abstract We previously reported that human muscle-derived stem cells (hMuStem cells) contribute to tissue repair after local administration into injured skeletal muscle or infarcted heart in immunodeficient rodent models. However, extrapolation of these findings to a clinical context is problematic owing to the considerable differences often seen between in vivo findings in humans versus rodents. Therefore, we investigated whether the muscle regenerative behavior of hMuStem cells is maintained in a clinically relevant transplantation context. Human MuStem cells were intramuscularly administered by high-density microinjection matrices into nonhuman primates receiving tacrolimus-based immunosuppression thereby reproducing the protocol that has so far produced the best results in clinical trials of cell therapy in myopathies. Four and 9 weeks after administration, histological analysis of cell injection sites revealed large numbers of hMuStem cell-derived nuclei in all cases. Most graft-derived nuclei were distributed in small myofiber groups in which no signs of a specific immune response were observed. Importantly, hMuStem cells contributed to simian tissue repair by fusing mainly with host myofibers, demonstrating their capacity for myofiber regeneration in this model. Together, these findings obtained in a valid preclinical model provide new insights supporting the potential of hMuStem cells in future cell therapies for muscle diseases.

Funder

Fonds Européen de Développement Régional

ANR

Agence Nationale de la Recherche

Jesse’s Journey Foundation for Gene and Cell Therapy of Canada

ANII

National Research and Innovation Agency

French Ministry of Higher Education, Research and Innovation

Publisher

Oxford University Press (OUP)

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