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Antibody targeting tumor-derived soluble NKG2D ligand sMIC reprograms NK cell homeostatic survival and function and enhances melanoma response to PDL1 blockade therapy

J Hematol Oncol. 2020; 
Fahmin Basher, Payal Dhar, Xin Wang, Derek A Wainwright, Bin Zhang, Jeffrey Sosman, Zhe Ji, Jennifer D Wu
Products/Services Used Details Operation
Peptide Synthesis … Lebanon, NH). In vivo NK cell-depleting anti-NK1.1 (clone PK136) and CD8 T cell-depleting antibody anti-CD8α (clone 2.43) were purchased from BioXcell. Peptide gp100 25-33 (KVPRNQDWL) was synthesized by GenScript. H-2D … Get A Quote

摘要

background: Melanoma patients who have detectable serum soluble NKG2D ligands either at the baseline or post-treatment of PD1/PDL1 blockade exhibit poor overall survival. Among families of soluble human NKG2D ligands, the soluble human MHC I chain-related molecule (sMIC) was found to be elevated in melanoma patients and mostly associated with poor response to PD1/PDL1 blockade therapy. methods: In this study, we aim to investigate whether co-targeting tumor-released sMIC enhances the therapeutic outcome of PD1/PDL1 blockade therapy for melanoma. We implanted sMIC-expressing B16F10 melanoma tumors into syngeneic host and evaluated therapeutic efficacy of anti-sMIC antibody and anti-PDL1 antibody combination ther... More

关键词

Anti-sMIC antibody, Melanoma, NKG2D ligands, PD1/PDL1 blockade, Soluble MHC I chain-related molecule (sMIC)