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W4321749285 endingPage "1989" @default.
W4321749285 startingPage "1975" @default.
W4321749285 abstract "Next-generation cancer immunotherapies may utilize immunostimulants to selectively activate the host immune system against tumor cells. Checkpoint inhibitors (CPIs) like anti-PD1/PDL-1 that inhibit immunosuppression have shown unprecedented success but are only effective in the 20-30% of patients that possess an already hot (immunogenic) tumor. In this regard, intratumoral (IT) injection of immunostimulants is a promising approach since they can work synergistically with CPIs to overcome the resistance to immunotherapies by inducing immune stimulation in the tumor. One such immunostimulant is granulocyte macrophage-colony-stimulating factor (GMCSF) that functions by recruiting and activating antigen-presenting cells (dendritic cells) in the tumor, thereby initiating anti-tumor immune responses. However, key problems with GMCSF are lack of efficacy and the risk of systemic toxicity caused by the leakage of GMCSF from the tumor tissue. We have designed tumor-retentive versions of GMCSF that are safe yet potent immunostimulants for the local treatment of solid tumors. The engineered GMCSFs (eGMCSF) were synthesized by recombinantly fusing tumor-ECM (extracellular matrix) binding peptides to GMCSF. The eGMCSFs exhibited enhanced tumor binding and potent immunological activity in vitro and in vivo. Upon IT administration, the tumor-retentive eGMCSFs persisted in the tumor, thereby alleviating systemic toxicity, and elicited localized immune activation to effectively turn an unresponsive immunologically cold tumor hot." @default.
W4321749285 created "2023-02-25" @default.
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W4321749285 date "2023-02-24" @default.
W4321749285 modified "2023-10-18" @default.
W4321749285 title "Design of a Tumor Binding GMCSF as Intratumoral Immunotherapy of Solid Tumors" @default.
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W4321749285 doi "https://doi.org/10.1021/acs.molpharmaceut.2c00897" @default.
W4321749285 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/36825806" @default.
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