2019
DOI: 10.1186/s40425-019-0794-7
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Longitudinal immune characterization of syngeneic tumor models to enable model selection for immune oncology drug discovery

Abstract: BackgroundThe ability to modulate immune-inhibitory pathways using checkpoint blockade antibodies such as αPD-1, αPD-L1, and αCTLA-4 represents a significant breakthrough in cancer therapy in recent years. This has driven interest in identifying small-molecule-immunotherapy combinations to increase the proportion of responses. Murine syngeneic models, which have a functional immune system, represent an essential tool for pre-clinical evaluation of new immunotherapies. However, immune response varies widely bet… Show more

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Cited by 77 publications
(72 citation statements)
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“…While syngeneic orthotopic models mimic more efficiently the disease biology of human disease, their main drawback relates to the monitoring of tumor progression, which requires the use of reporter genes, invasive surgical procedures or imaging methods such as real-time in-life fluorescence and bioluminescence imaging. Despite these limitations, syngeneic mouse models offer clues and proofs of concept in immunocompetent hosts and thereby represent an excellent preclinical platform to test compounds based on immuno-oncology targets to treat cancer [ 11 ].…”
Section: Introductionmentioning
confidence: 99%
“…While syngeneic orthotopic models mimic more efficiently the disease biology of human disease, their main drawback relates to the monitoring of tumor progression, which requires the use of reporter genes, invasive surgical procedures or imaging methods such as real-time in-life fluorescence and bioluminescence imaging. Despite these limitations, syngeneic mouse models offer clues and proofs of concept in immunocompetent hosts and thereby represent an excellent preclinical platform to test compounds based on immuno-oncology targets to treat cancer [ 11 ].…”
Section: Introductionmentioning
confidence: 99%
“…Undoubtedly, the formation of transplanted tumors is different from tumors originating de novo. Moreover, the tumor microenvironment will be mostly determined by the local innate immune response triggered by injection-induced inflammation and the presence of a large number of tumor cells [23,24]. Usually, tumor cells are injected subcutaneously, as it is easier to track tumor development [25].…”
Section: Syngeneic Tumor Modelsmentioning
confidence: 99%
“…After the lack of cooperation between HCA-EFZP-aPDL1 and the treatments described above in the PC model, we targeted other potential sources of tumor resistance such as macrophages. The MC38 tumor model is characterized by a diverse composition of the leukocyte infiltrate, with a progressive expansion of macrophages and a concomitant reduction in their pro-inflammatory (M1) phenotype [23]. They present reduced IL-12 and iNOS signaling, and activation of the IL-10 pathway [24].…”
Section: Depletion Of Macrophages Increases the Survival Of Mice Treated With Hca-efzp-apdl1mentioning
confidence: 99%