Effects of leukapheresis protocol, cell processing and cryopreservation on the generation of monocyte-derived DC for immune therapy
Contribuinte(s) |
J. Barrett |
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Data(s) |
01/01/2003
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Resumo |
Background Many clinical trials of DC-based immunotherapy involve administration of monocyte-derived DCs (Mo-DC) on multiple occasions. We aimed to determine the optimal cell processing procedures and timing (leukapheresis, RBC depletion and cryopreservation) for generation of Mo-DC for clinical purposes. Methods Leukapheresis was undertaken using a COBE Spectra. Two instrument settings were compared - the standard semi-automated software (Version 4.7) (n = 10) and the fully automated software (Version 6.0) (n = 40). Density gradient centrifugation using Ficoll, Percoll, a combination of these methods or neither for RBC depletion were compared. Outcomes (including cell yield and purity) were compared for cryopreserved unmanipulated monocytes and cryopreserved Mo-DC. Results Software Version 6.0 provided significantly better enrichment for monocytes (P |
Identificador | |
Idioma(s) |
eng |
Publicador |
Taylor & Francis |
Palavras-Chave | #Biotechnology & Applied Microbiology #Cell Biology #Hematology #Medicine, Research & Experimental #Monocyte Derived Dendritic Cells #Cellular Immune Therapy #Leukapheresis #C1 #320202 Cellular Immunology #730107 Inherited diseases (incl. gene therapy) |
Tipo |
Journal Article |