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A technique for removing tumourigenic pluripotent stem cells using rBC2LCN lectin

INTRODUCTION: Tumourigenesis attributed to residual undifferentiated cells in a graft is considered to be a significant issue in cell therapy using human pluripotent stem cells. To ensure the safety of regenerative medicine derived from pluripotent stem cells, residual undifferentiated cells must be...

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Autores principales: Haramoto, Yoshikazu, Onuma, Yasuko, Mawaribuchi, Shuuji, Nakajima, Yoshiro, Aiki, Yasuhiko, Higuchi, Kumiko, Shimizu, Madoka, Tateno, Hiroaki, Hirabayashi, Jun, Ito, Yuzuru
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Japanese Society for Regenerative Medicine 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7240284/
https://www.ncbi.nlm.nih.gov/pubmed/32462059
http://dx.doi.org/10.1016/j.reth.2020.03.017
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author Haramoto, Yoshikazu
Onuma, Yasuko
Mawaribuchi, Shuuji
Nakajima, Yoshiro
Aiki, Yasuhiko
Higuchi, Kumiko
Shimizu, Madoka
Tateno, Hiroaki
Hirabayashi, Jun
Ito, Yuzuru
author_facet Haramoto, Yoshikazu
Onuma, Yasuko
Mawaribuchi, Shuuji
Nakajima, Yoshiro
Aiki, Yasuhiko
Higuchi, Kumiko
Shimizu, Madoka
Tateno, Hiroaki
Hirabayashi, Jun
Ito, Yuzuru
author_sort Haramoto, Yoshikazu
collection PubMed
description INTRODUCTION: Tumourigenesis attributed to residual undifferentiated cells in a graft is considered to be a significant issue in cell therapy using human pluripotent stem cells. To ensure the safety of regenerative medicine derived from pluripotent stem cells, residual undifferentiated cells must be eliminated in the manufacturing process. We previously described the lectin probe rBC2LCN, which binds harmlessly and specifically to the cell surface of human pluripotent stem cells. We report here a technique using rBC2LCN to remove pluripotent cells from a heterogenous population to reduce the chance of teratoma formation. METHODS: We demonstrate a method for separating residual tumourigenic cells using rBC2LCN-bound magnetic beads. This technology is a novel use of their previous discovery that rBC2LCN is a lectin that selectively binds to pluripotent cells. We optimize and validate a method to remove hPSCs from a mixture with human fibroblasts using rBC2LCN-conjugated magnetic beads. RESULTS: Cells with the potential to form teratoma could be effectively eliminated from a heterogeneous cell population with biotin-labelled rBC2LCN and streptavidin-bound magnetic beads. The efficiency was measured by FACS, ddPCR, and animal transplantation, suggesting that magnetic cell separation using rBC2LCN is quite efficient for eliminating hPSCs from mixed cell populations. CONCLUSIONS: The removal of residual tumourigenic cells based on rBC2LCN could be a practical option for laboratory use and industrialisation of regenerative medicine using human pluripotent stem cells.
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spelling pubmed-72402842020-05-26 A technique for removing tumourigenic pluripotent stem cells using rBC2LCN lectin Haramoto, Yoshikazu Onuma, Yasuko Mawaribuchi, Shuuji Nakajima, Yoshiro Aiki, Yasuhiko Higuchi, Kumiko Shimizu, Madoka Tateno, Hiroaki Hirabayashi, Jun Ito, Yuzuru Regen Ther Original Article INTRODUCTION: Tumourigenesis attributed to residual undifferentiated cells in a graft is considered to be a significant issue in cell therapy using human pluripotent stem cells. To ensure the safety of regenerative medicine derived from pluripotent stem cells, residual undifferentiated cells must be eliminated in the manufacturing process. We previously described the lectin probe rBC2LCN, which binds harmlessly and specifically to the cell surface of human pluripotent stem cells. We report here a technique using rBC2LCN to remove pluripotent cells from a heterogenous population to reduce the chance of teratoma formation. METHODS: We demonstrate a method for separating residual tumourigenic cells using rBC2LCN-bound magnetic beads. This technology is a novel use of their previous discovery that rBC2LCN is a lectin that selectively binds to pluripotent cells. We optimize and validate a method to remove hPSCs from a mixture with human fibroblasts using rBC2LCN-conjugated magnetic beads. RESULTS: Cells with the potential to form teratoma could be effectively eliminated from a heterogeneous cell population with biotin-labelled rBC2LCN and streptavidin-bound magnetic beads. The efficiency was measured by FACS, ddPCR, and animal transplantation, suggesting that magnetic cell separation using rBC2LCN is quite efficient for eliminating hPSCs from mixed cell populations. CONCLUSIONS: The removal of residual tumourigenic cells based on rBC2LCN could be a practical option for laboratory use and industrialisation of regenerative medicine using human pluripotent stem cells. Japanese Society for Regenerative Medicine 2020-05-19 /pmc/articles/PMC7240284/ /pubmed/32462059 http://dx.doi.org/10.1016/j.reth.2020.03.017 Text en © 2020 The Japanese Society for Regenerative Medicine. Production and hosting by Elsevier B.V. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Article
Haramoto, Yoshikazu
Onuma, Yasuko
Mawaribuchi, Shuuji
Nakajima, Yoshiro
Aiki, Yasuhiko
Higuchi, Kumiko
Shimizu, Madoka
Tateno, Hiroaki
Hirabayashi, Jun
Ito, Yuzuru
A technique for removing tumourigenic pluripotent stem cells using rBC2LCN lectin
title A technique for removing tumourigenic pluripotent stem cells using rBC2LCN lectin
title_full A technique for removing tumourigenic pluripotent stem cells using rBC2LCN lectin
title_fullStr A technique for removing tumourigenic pluripotent stem cells using rBC2LCN lectin
title_full_unstemmed A technique for removing tumourigenic pluripotent stem cells using rBC2LCN lectin
title_short A technique for removing tumourigenic pluripotent stem cells using rBC2LCN lectin
title_sort technique for removing tumourigenic pluripotent stem cells using rbc2lcn lectin
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7240284/
https://www.ncbi.nlm.nih.gov/pubmed/32462059
http://dx.doi.org/10.1016/j.reth.2020.03.017
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