2008
DOI: 10.3324/haematol.12349
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A bioluminescence imaging based in vivo model for preclinical testing of novel cellular immunotherapy strategies to improve the graft-versus-myeloma effect

Abstract: BackgroundThe development and preclinical testing of novel immunotherapy strategies for multiple myeloma can benefit substantially from a humanized animal model that enables quantitative realtime monitoring of tumor progression. Here we have explored the feasibility of establishing such a model in immunodeficient RAG2

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Cited by 39 publications
(66 citation statements)
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“…To examine whether these characteristics translated into anti-tumor efficacy in vivo, we evaluated daratumumab in two mouse xenograft tumor models, based on Daudi lymphoma and UM-9 multiple myeloma cells stably expressing the luciferase gene (19,20).…”
Section: Induction Of Adcc Against MM Cellsmentioning
confidence: 99%
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“…To examine whether these characteristics translated into anti-tumor efficacy in vivo, we evaluated daratumumab in two mouse xenograft tumor models, based on Daudi lymphoma and UM-9 multiple myeloma cells stably expressing the luciferase gene (19,20).…”
Section: Induction Of Adcc Against MM Cellsmentioning
confidence: 99%
“…For the mouse UM9 tumor xenograft model, experiments were performed essentially as decribed by Rozemuller et al (20). Briefly, 20 3 10 6 UM9-luc cells were injected i.v.…”
Section: Mouse Tumor Xenograft Modelsmentioning
confidence: 99%
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“…Daudi cells were transfected with gWIZ luciferase as previously described 16 (Daudi-luc). The MM cell lines UM-9, generated at the University Medical Center (Utrecht, the Netherlands), 45 and L363, obtained from the ATCC and gene-marked with GFP and luciferase marker genes, 46 were transduced with human CD38 gene to obtain CD38 expression levels comparable to primary myeloma cells. For this, the amphotropic Phoenix packaging cell line (Phoenix Ampho) was transfected, using calcium phosphate precipitation, with the pQCXIN vector in which the gene encoding human CD38 was inserted.…”
Section: Cell Linesmentioning
confidence: 99%
“…When inoculating the less immunogenic MM cell line RPMI-8226/S, the GvM response was poor. Nevertheless, these mice developed GvHD, underlining that less immunogenic tumors can evade the GvM response despite the occurrence of GvHD [83]. Another xenogeneic GvM model has been described by Freeman et al After injection of GFP/luciferase-transfected human RPMI8226 human MM cells into CD122-depleted NOD-SCID mice, they obtained a MM model with bone marrow infiltration and bone lesions.…”
Section: Allogeneic Transplantation In Immunocompetent Murine MM Modelsmentioning
confidence: 99%