Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.

Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.

Human amniotic epithelial cells (hAEC) isolated from term placenta have stem cell-like properties, differentiate into tissue specific cells and reduce lung and liver inflammation and fibrosis following transplantation into disease models established in mice. These features together with their low im...

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Main Authors: Gita Pratama, Vijesh Vaghjiani, Jing Yang Tee, Yu Han Liu, James Chan, Charmaine Tan, Padma Murthi, Caroline Gargett, Ursula Manuelpillai
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/22073147/?tool=EBI
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spelling doaj-dfa4d0631dd9448a8aa0be3f063f1e292021-06-19T05:05:53ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-01-01611e2613610.1371/journal.pone.0026136Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.Gita PratamaVijesh VaghjianiJing Yang TeeYu Han LiuJames ChanCharmaine TanPadma MurthiCaroline GargettUrsula ManuelpillaiHuman amniotic epithelial cells (hAEC) isolated from term placenta have stem cell-like properties, differentiate into tissue specific cells and reduce lung and liver inflammation and fibrosis following transplantation into disease models established in mice. These features together with their low immunogenicity and immunosuppressive properties make hAEC an attractive source of cells for potential therapeutic applications. However, generation of large cell numbers required for therapies through serial expansion in xenobiotic-free media may be a limiting factor. We investigated if hAEC could be expanded in xenobiotic-free media and if expansion altered their differentiation capacity, immunophenotype, immunosuppressive properties and production of immunomodulatory factors. Serial expansion in xenobiotic-free media was limited with cumulative cell numbers and population doubling times significantly lower than controls maintained in fetal calf serum. The epithelial morphology of primary hAEC changed into mesenchymal-stromal like cells by passage 4-5 (P4-P5) with down regulation of epithelial markers CK7, CD49f, EpCAM and E-cadherin and elevation of mesenchymal-stromal markers CD44, CD105, CD146 and vimentin. The P5 hAEC expanded in xenobiotic-free medium differentiated into osteocyte and alveolar epithelium-like cells, but not chondrocyte, hepatocyte, α- and β-pancreatic-like cells. Expression of HLA Class IA, Class II and co-stimulatory molecules CD80, CD86 and CD40 remained unaltered. The P5 hAEC suppressed mitogen stimulated T cell proliferation, but were less suppressive compared with primary hAEC at higher splenocyte ratios. Primary and P5 hAEC did not secrete the immunosuppressive factors IL-10 and HGF, whereas TGF-β1 and HLA-G were reduced and IL-6 elevated in P5 hAEC. These findings suggest that primary and expanded hAEC may be suitable for different cellular therapeutic applications.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/22073147/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Gita Pratama
Vijesh Vaghjiani
Jing Yang Tee
Yu Han Liu
James Chan
Charmaine Tan
Padma Murthi
Caroline Gargett
Ursula Manuelpillai
spellingShingle Gita Pratama
Vijesh Vaghjiani
Jing Yang Tee
Yu Han Liu
James Chan
Charmaine Tan
Padma Murthi
Caroline Gargett
Ursula Manuelpillai
Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.
PLoS ONE
author_facet Gita Pratama
Vijesh Vaghjiani
Jing Yang Tee
Yu Han Liu
James Chan
Charmaine Tan
Padma Murthi
Caroline Gargett
Ursula Manuelpillai
author_sort Gita Pratama
title Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.
title_short Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.
title_full Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.
title_fullStr Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.
title_full_unstemmed Changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.
title_sort changes in culture expanded human amniotic epithelial cells: implications for potential therapeutic applications.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2011-01-01
description Human amniotic epithelial cells (hAEC) isolated from term placenta have stem cell-like properties, differentiate into tissue specific cells and reduce lung and liver inflammation and fibrosis following transplantation into disease models established in mice. These features together with their low immunogenicity and immunosuppressive properties make hAEC an attractive source of cells for potential therapeutic applications. However, generation of large cell numbers required for therapies through serial expansion in xenobiotic-free media may be a limiting factor. We investigated if hAEC could be expanded in xenobiotic-free media and if expansion altered their differentiation capacity, immunophenotype, immunosuppressive properties and production of immunomodulatory factors. Serial expansion in xenobiotic-free media was limited with cumulative cell numbers and population doubling times significantly lower than controls maintained in fetal calf serum. The epithelial morphology of primary hAEC changed into mesenchymal-stromal like cells by passage 4-5 (P4-P5) with down regulation of epithelial markers CK7, CD49f, EpCAM and E-cadherin and elevation of mesenchymal-stromal markers CD44, CD105, CD146 and vimentin. The P5 hAEC expanded in xenobiotic-free medium differentiated into osteocyte and alveolar epithelium-like cells, but not chondrocyte, hepatocyte, α- and β-pancreatic-like cells. Expression of HLA Class IA, Class II and co-stimulatory molecules CD80, CD86 and CD40 remained unaltered. The P5 hAEC suppressed mitogen stimulated T cell proliferation, but were less suppressive compared with primary hAEC at higher splenocyte ratios. Primary and P5 hAEC did not secrete the immunosuppressive factors IL-10 and HGF, whereas TGF-β1 and HLA-G were reduced and IL-6 elevated in P5 hAEC. These findings suggest that primary and expanded hAEC may be suitable for different cellular therapeutic applications.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/22073147/?tool=EBI
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