Clinical-grade allogeneic amniotic fluid stem cell banking: quality control for therapeutic applications and drug development

Phermthai T.; Thongbopit S.; Wataganara T.; Wichitwiengrat S.; Chuaynarong P.; Poothong J.; Auewarakul P.

Clinical-grade allogeneic amniotic fluid stem cell banking: quality control for therapeutic applications and drug development

2

Issued Date

2025-09-26

Resource Type

Article

eISSN

17576512

DOI

10.1186/s13287-025-04654-2

Scopus ID

2-s2.0-105017416377

Pubmed ID

41013842

Journal Title

Stem Cell Research Therapy

Volume

16

Issue

1

Rights Holder(s)

SCOPUS

Bibliographic Citation

Stem Cell Research Therapy Vol.16 No.1 (2025) , 509

Suggested Citation

Phermthai T., Thongbopit S., Wataganara T., Wichitwiengrat S., Chuaynarong P., Poothong J., Auewarakul P. Clinical-grade allogeneic amniotic fluid stem cell banking: quality control for therapeutic applications and drug development. Stem Cell Research Therapy Vol.16 No.1 (2025) , 509. doi:10.1186/s13287-025-04654-2 Retrieved from: https://repository.li.mahidol.ac.th/handle/123456789/112463

Title

Clinical-grade allogeneic amniotic fluid stem cell banking: quality control for therapeutic applications and drug development

Author(s)

Phermthai T.
Thongbopit S.
Wataganara T.
Wichitwiengrat S.
Chuaynarong P.
Poothong J.
Auewarakul P.

Author's Affiliation

Siriraj Hospital

Corresponding Author(s)

Phermthai T.

Other Contributor(s)

Mahidol University

Abstract

BACKGROUND: Allogeneic mesenchymal stem cells (MSCs) offer significant advantages for various medical treatments. However, maintaining an allogeneic MSC bank presents challenges due to concerns about heterogeneity, which directly affects their efficacy. Additionally, issues related to cell senescence can arise even after a short period of serial passaging. Amniotic fluid mesenchymal stem cells (AF-MSCs) demonstrate greater proliferation efficiency compared to other MSCs. They can form clonal cell lines that generate a homogeneous population and can expand in long-term cultures without undergoing cellular senescence. Therefore, this study introduces a method for establishing cell lines and a banking system for AF-MSCs, providing high-quality, authentic human MSCs for clinical applications. METHODS: In this research, we isolated clonal AF-MSCs to select them for the creation of AF-MSC stock through long-term serial passaging. We developed a three-tier cell banking system, which includes an AF-MSC stock, a Master Cell Bank at passage 4, and a Working Cell Bank at passage 9. Standard characteristics were employed to verify identity, safety, and quality control assessments. RESULTS: Three out of twelve AF-MSC clones were selected to exemplify cell line establishment, the creation of a three-tier banking system, and quality control evaluations to determine their suitability for clinical-grade cell lines in medical applications. CONCLUSIONS: This study offers a comprehensive technical and translational overview of establishing an allogeneic amniotic fluid mesenchymal stem cell bank, tailored for medical applications and drug development.

Keyword(s)

Biochemistry, Genetics and Molecular Biology
Medicine

URI

https://repository.li.mahidol.ac.th/handle/123456789/112463

Collections

Scopus 2025

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