Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.

Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.

Abundance and accessibility render skin-derived stem cells an attractive cell source for tissue engineering applications. Toward assessing their utility, the variability of constructs engineered from human dermis-isolated adult stem (hDIAS) cells was examined with respect to different anatomical loc...

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Main Authors: Heenam Kwon, Anne K Haudenschild, Wendy E Brown, Natalia Vapniarsky, Nikolaos K Paschos, Boaz Arzi, Jerry C Hu, Kyriacos A Athanasiou
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5540597?pdf=render
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spelling doaj-9458cb2bd2a0496eaff2bf17926f84482020-11-25T01:57:36ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-01128e018253110.1371/journal.pone.0182531Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.Heenam KwonAnne K HaudenschildWendy E BrownNatalia VapniarskyNikolaos K PaschosBoaz ArziJerry C HuKyriacos A AthanasiouAbundance and accessibility render skin-derived stem cells an attractive cell source for tissue engineering applications. Toward assessing their utility, the variability of constructs engineered from human dermis-isolated adult stem (hDIAS) cells was examined with respect to different anatomical locations (foreskin, breast, and abdominal skin), both in vitro and in a subcutaneous, athymic mouse model. All anatomical locations yielded hDIAS cells with multi-lineage differentiation potentials, though adipogenesis was not seen for foreskin-derived hDIAS cells. Using engineered cartilage as a model, tissue engineered constructs from hDIAS cells were compared. Construct morphology differed by location. The mechanical properties of human foreskin- and abdominal skin-derived constructs were similar at implantation, remaining comparable after 4 additional weeks of culture in vivo. Breast skin-derived constructs were not mechanically testable. For all groups, no signs of abnormality were observed in the host. Addition of aggregate redifferentiation culture prior to construct formation improved chondrogenic differentiation of foreskin-derived hDIAS cells, as evident by increases in glycosaminoglycan and collagen contents. More robust Alcian blue staining and homogeneous cell populations were also observed compared to controls. Human DIAS cells elicited no adverse host responses, reacted positively to chondrogenic regimens, and possessed multi-lineage differentiation potential with the caveat that efficacy may differ by anatomical origin of the skin. Taken together, these results suggest that hDIAS cells hold promise as a potential cell source for a number of tissue engineering applications.http://europepmc.org/articles/PMC5540597?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Heenam Kwon
Anne K Haudenschild
Wendy E Brown
Natalia Vapniarsky
Nikolaos K Paschos
Boaz Arzi
Jerry C Hu
Kyriacos A Athanasiou
spellingShingle Heenam Kwon
Anne K Haudenschild
Wendy E Brown
Natalia Vapniarsky
Nikolaos K Paschos
Boaz Arzi
Jerry C Hu
Kyriacos A Athanasiou
Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.
PLoS ONE
author_facet Heenam Kwon
Anne K Haudenschild
Wendy E Brown
Natalia Vapniarsky
Nikolaos K Paschos
Boaz Arzi
Jerry C Hu
Kyriacos A Athanasiou
author_sort Heenam Kwon
title Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.
title_short Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.
title_full Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.
title_fullStr Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.
title_full_unstemmed Tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.
title_sort tissue engineering potential of human dermis-isolated adult stem cells from multiple anatomical locations.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description Abundance and accessibility render skin-derived stem cells an attractive cell source for tissue engineering applications. Toward assessing their utility, the variability of constructs engineered from human dermis-isolated adult stem (hDIAS) cells was examined with respect to different anatomical locations (foreskin, breast, and abdominal skin), both in vitro and in a subcutaneous, athymic mouse model. All anatomical locations yielded hDIAS cells with multi-lineage differentiation potentials, though adipogenesis was not seen for foreskin-derived hDIAS cells. Using engineered cartilage as a model, tissue engineered constructs from hDIAS cells were compared. Construct morphology differed by location. The mechanical properties of human foreskin- and abdominal skin-derived constructs were similar at implantation, remaining comparable after 4 additional weeks of culture in vivo. Breast skin-derived constructs were not mechanically testable. For all groups, no signs of abnormality were observed in the host. Addition of aggregate redifferentiation culture prior to construct formation improved chondrogenic differentiation of foreskin-derived hDIAS cells, as evident by increases in glycosaminoglycan and collagen contents. More robust Alcian blue staining and homogeneous cell populations were also observed compared to controls. Human DIAS cells elicited no adverse host responses, reacted positively to chondrogenic regimens, and possessed multi-lineage differentiation potential with the caveat that efficacy may differ by anatomical origin of the skin. Taken together, these results suggest that hDIAS cells hold promise as a potential cell source for a number of tissue engineering applications.
url http://europepmc.org/articles/PMC5540597?pdf=render
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