GMP-compliant iPS cell lines show widespread plasticity in a new set of differentiation workflows for cell replacement and cancer immunotherapy

Autor(en): Terheyden-Keighley, D.
Hühne, M.
Berger, T.
Hiller, B.
Martins, S.
Gamerschlag, A.
Sabour, D.
Meffert, A.
Kislat, A.
Slotta, C.
Hafezi, F.
Lichte, J.
Sudheer, S.
Tessmer, K.
Psathaki, Katherina 
Ader, M.
Kogler, G.
Greber, B.
Stichwörter: article; cancer immunotherapy; CD34 antigen; CD34 selection; Cell Proliferation; cell survival; cell therapy; chondrocyte; cytotoxicity; dendritic cell; DNA repair; dorsomorphin; electric resistance; flow cytometry; gene editing; gene expression; gene targeting; good manufacturing practice; hemangioblast; hematopoietic stem cell; human; immunofluorescence; immunofluorescence microscopy; immunotherapy; induced pluripotent stem cell; interleukin 15; interleukin 3; interleukin 7; macrophage; melanosome; mesenchymal stroma cell; mesenchyme cell; monocyte; mutational load; myocarditis; natural killer T cell; neural stem cell; nuclear reprogramming; nucleotide sequence; plasticity; pluripotent stem cell; retinal pigment epithelium; reverse transcription polymerase chain reaction; RNA sequence; stroma cell; transforming growth factor beta; umbilical cord blood; Wnt signaling
Erscheinungsdatum: 2024
Herausgeber: Oxford University Press
Enthalten in: Stem Cells Translational Medicine
Band: 13
Ausgabe: 9
Startseite: 898
Seitenende: 911
ISSN: 2157-6564
DOI: 10.1093/stcltm/szae047
Externe URL: https://www.scopus.com/inward/record.uri?eid=2-s2.0-85204069874&doi=10.1093%2fstcltm%2fszae047&partnerID=40&md5=a271b17240cb73898c6661df55014731

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