Good Manufacturing Practice–compliant human induced pluripotent stem cells: from bench to putative clinical products

Few human induced pluripotent stem cell (hiPSC) lines are Good Manufacturing Practice (GMP)-compliant, limiting the clinical use of hiPSC-derived products. Here, we addressed this by establishing and validating an in-house platform to produce GMP-compliant hiPSCs that would be appropriate for produc...

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Veröffentlicht in:Cytotherapy (Oxford, England) England), 2024-06, Vol.26 (6), p.556-566
Hauptverfasser: Novoa, Juan J., Westra, Inge M., Steeneveld, Esther, Fonseca Neves, Natascha, Arendzen, Christiaan H., Rajaei, Bahareh, Grundeken, Esmée, Yildiz, Mehmet, van der Valk, Wouter, Salvador, Alison, Carlotti, Françoise, Dijkers, Pascale F., Locher, Heiko, van den Berg, Cathelijne W., Raymond, Karine I., Kirkeby, Agnete, Mummery, Christine L., Rabelink, Ton J., Freund, Christian, Meij, Pauline, Wieles, Brigitte
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Sprache:eng
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Zusammenfassung:Few human induced pluripotent stem cell (hiPSC) lines are Good Manufacturing Practice (GMP)-compliant, limiting the clinical use of hiPSC-derived products. Here, we addressed this by establishing and validating an in-house platform to produce GMP-compliant hiPSCs that would be appropriate for producing both allogeneic and autologous hiPSC-derived products. Our standard research protocol for hiPSCs production was adapted and translated into a GMP-compliant platform. In addition to the generation of GMP-compliant hiPSC, the platform entails the methodology for donor recruitment, consent and screening, donor material procurement, hiPSCs manufacture, in-process control, specific QC test validation, QC testing, product release, hiPSCs storage and stability testing. For platform validation, one test run and three production runs were performed. Highest-quality lines were selected to establish master cell banks (MCBs). Two MCBs were successfully released under GMP conditions. They demonstrated safety (sterility, negative mycoplasma, endotoxins 75% of cells expressing markers of undifferentiated state, identical STR profile, normal karyotype in >20 metaphases), purity (negative residual vectors and no plasmid integration in the genome) and potency (expression of at least two of the three markers for each of the three germ layers). In addition, directed differentiation to somitoids (skeletal muscle precursors) and six potential clinical products from all three germ layers was achieved: pancreatic islets (endoderm), kidney organoids and cardiomyocytes (mesoderm), and keratinocytes, GABAergic interneurons and inner-ear organoids (ectoderm). We successfully developed and validated a platform for generating GMP-compliant hiPSC lines. The two MCBs released were shown to differentiate into clinical products relevant for our own and other regenerative medicine interests. [Display omitted]
ISSN:1465-3249
1477-2566
DOI:10.1016/j.jcyt.2024.02.021