Therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution

Skeletal muscle makes up 40–50% of body mass, and is thus considered to be a good adult stem cell source for autologous therapy. Although, several stem/progenitor cells have been fractionated from mouse skeletal muscle showing a high potential for therapeutic use, it is unclear whether this is the c...

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Autores principales: Tamaki, Tetsuro, Uchiyama, Yoshiyasu, Hirata, Maki, Hashimoto, Hiroyuki, Nakajima, Nobuyuki, Saito, Kosuke, Terachi, Toshiro, Mochida, Joji
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2015
Materias:
Physiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4451695/
https://www.ncbi.nlm.nih.gov/pubmed/26082721
http://dx.doi.org/10.3389/fphys.2015.00165
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author Tamaki, Tetsuro
Uchiyama, Yoshiyasu
Hirata, Maki
Hashimoto, Hiroyuki
Nakajima, Nobuyuki
Saito, Kosuke
Terachi, Toshiro
Mochida, Joji
author_facet Tamaki, Tetsuro
Uchiyama, Yoshiyasu
Hirata, Maki
Hashimoto, Hiroyuki
Nakajima, Nobuyuki
Saito, Kosuke
Terachi, Toshiro
Mochida, Joji
author_sort Tamaki, Tetsuro
collection PubMed
description Skeletal muscle makes up 40–50% of body mass, and is thus considered to be a good adult stem cell source for autologous therapy. Although, several stem/progenitor cells have been fractionated from mouse skeletal muscle showing a high potential for therapeutic use, it is unclear whether this is the case in human. Differentiation and therapeutic potential of human skeletal muscle-derived cells (Sk-Cs) was examined. Samples (5–10 g) were obtained from the abdominal and leg muscles of 36 patients (age, 17–79 years) undergoing prostate cancer treatment or leg amputation surgery. All patients gave informed consent. Sk-Cs were isolated using conditioned collagenase solution, and were then sorted as CD34(−)/CD45(−)/CD29(+) (Sk-DN/29(+)) and CD34(+)/CD45(−) (Sk-34) cells, in a similar manner as for the previous mouse Sk-Cs. Both cell fractions were appropriately expanded using conditioned culture medium for about 2 weeks. Differentiation potentials were then examined during cell culture and in vivo transplantation into the severely damaged muscles of athymic nude mice and rats. Interestingly, these two cell fractions could be divided into highly myogenic (Sk-DN/29(+)) and multipotent stem cell (Sk-34) fractions, in contrast to mouse Sk-Cs, which showed comparable capacities in both cells. At 6 weeks after the separate transplantation of both cell fractions, the former showed an active contribution to muscle fiber regeneration, but the latter showed vigorous engraftment to the interstitium associated with differentiation into Schwann cells, perineurial/endoneurial cells, and vascular endothelial cells and pericytes, which corresponded to previous observations with mouse SK-Cs. Importantly, mixed cultures of both cells resulted the reduction of tissue reconstitution capacities in vivo, whereas co-transplantation after separate expansion showed favorable results. Therefore, human Sk-Cs are potentially applicable to therapeutic autografts and show multiple differentiation potential in vivo.
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spelling pubmed-44516952015-06-16 Therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution Tamaki, Tetsuro Uchiyama, Yoshiyasu Hirata, Maki Hashimoto, Hiroyuki Nakajima, Nobuyuki Saito, Kosuke Terachi, Toshiro Mochida, Joji Front Physiol Physiology Skeletal muscle makes up 40–50% of body mass, and is thus considered to be a good adult stem cell source for autologous therapy. Although, several stem/progenitor cells have been fractionated from mouse skeletal muscle showing a high potential for therapeutic use, it is unclear whether this is the case in human. Differentiation and therapeutic potential of human skeletal muscle-derived cells (Sk-Cs) was examined. Samples (5–10 g) were obtained from the abdominal and leg muscles of 36 patients (age, 17–79 years) undergoing prostate cancer treatment or leg amputation surgery. All patients gave informed consent. Sk-Cs were isolated using conditioned collagenase solution, and were then sorted as CD34(−)/CD45(−)/CD29(+) (Sk-DN/29(+)) and CD34(+)/CD45(−) (Sk-34) cells, in a similar manner as for the previous mouse Sk-Cs. Both cell fractions were appropriately expanded using conditioned culture medium for about 2 weeks. Differentiation potentials were then examined during cell culture and in vivo transplantation into the severely damaged muscles of athymic nude mice and rats. Interestingly, these two cell fractions could be divided into highly myogenic (Sk-DN/29(+)) and multipotent stem cell (Sk-34) fractions, in contrast to mouse Sk-Cs, which showed comparable capacities in both cells. At 6 weeks after the separate transplantation of both cell fractions, the former showed an active contribution to muscle fiber regeneration, but the latter showed vigorous engraftment to the interstitium associated with differentiation into Schwann cells, perineurial/endoneurial cells, and vascular endothelial cells and pericytes, which corresponded to previous observations with mouse SK-Cs. Importantly, mixed cultures of both cells resulted the reduction of tissue reconstitution capacities in vivo, whereas co-transplantation after separate expansion showed favorable results. Therefore, human Sk-Cs are potentially applicable to therapeutic autografts and show multiple differentiation potential in vivo. Frontiers Media S.A. 2015-06-02 /pmc/articles/PMC4451695/ /pubmed/26082721 http://dx.doi.org/10.3389/fphys.2015.00165 Text en Copyright © 2015 Tamaki, Uchiyama, Hirata, Hashimoto, Nakajima, Saito, Terachi and Mochida. http://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) or licensor 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 Physiology
Tamaki, Tetsuro
Uchiyama, Yoshiyasu
Hirata, Maki
Hashimoto, Hiroyuki
Nakajima, Nobuyuki
Saito, Kosuke
Terachi, Toshiro
Mochida, Joji
Therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution
title Therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution
title_full Therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution
title_fullStr Therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution
title_full_unstemmed Therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution
title_short Therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution
title_sort therapeutic isolation and expansion of human skeletal muscle-derived stem cells for the use of muscle-nerve-blood vessel reconstitution
topic Physiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4451695/
https://www.ncbi.nlm.nih.gov/pubmed/26082721
http://dx.doi.org/10.3389/fphys.2015.00165
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