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Enhancement Of T-Cell Immunity To Osteosarcoma By Modulation Of Programmed Death Receptor Pathway Pooja Hingorani, Danielle Lussier, Joseph Blattman
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Overview T cell tolerance and immune inhibitory pathways in osteosarcoma Review our data
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Immune tolerance in osteosarcoma Loss of Class I HLA expression in osteosarcoma tumors related to worse overall survival* CTLA4 polymorphisms are associated with higher risk of developing osteosarcoma** Metastatic osteosarcoma expresses T cell Ig/mucin molecule 3 (TIM3), which in other tumor settings inhibits the function of infiltrating CTL, leading to tumor progression # B7-H3 expression, a co-inhibitory protein involved in tumor immune escape from T cells, inversely correlates with CTL infiltration in human osteosarcoma, and is indicative of poor prognosis in osteosarcoma patients @ *Tshukahara et al., Cancer Sci 2006; **Liu et al, DNA Cell Bio 2011; #Shang et al., Oncol Lett 2013; @ Wang et al., Plos One 2013
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Relative expression of PDL1 in osteosarcoma Shen J K et al. Cancer Immunol Res 2014;2:690-698 ©2014 by American Association for Cancer Research
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Overall survival of 37 patients with osteosarcoma in relation to PDL1 gene expression. Shen J K et al. Cancer Immunol Res 2014;2:690-698 ©2014 by American Association for Cancer Research
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Characterization of the origins of metastases. Shen J K et al. Cancer Immunol Res 2014;2:690-698 ©2014 by American Association for Cancer Research
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Specific Aims Evaluate expression of PD-L1 on tumor cells and PD-1 on TILs in patient samples and metastatic osteosarcoma cell line (in vitro and in vivo) Evaluate the functional ability of TILs infiltrating metastatic tumors Evaluate the effect of PD-L1 blockade on development and progression of pulmonary metastases in vivo Evaluate the effect of combinational therapies (PD-L1 antibody + chemotherapy; PD-L1 antibody + ipilimumab)
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PD-L1 is expressed in human metastatic osteosarcoma 50um Isotype Metastatic Osteosarcoma PD-L1 Primary Osteosarcoma 50um 12/ 16 (75% ) of metastatic tumors had some PD-L1 expression
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PD-1 is expressed on human metastatic TILs 50um Isotype PD-1 50um Metastatic Osteosarcoma Primary Osteosarcoma -13/16 (81%) of metastatic tumors had PD-1+ TILs -In 11/16 (70%) metastatic tumors, PD-1 expression on TILs correlated with PD-L1 expression on tumor cells
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PD-L1 expression is increased in K7M2 osteosarcoma cells PD-L1 % of Maximum 4073 1848 Pre Implantation Post Tumor 30%
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TILs from lung metastases are PD-1+ %PD1+ SPLEEN CD8TIL CD8 * CD8 PD-1 SPLEENTIL 94% 6% 87% 13% Isotype PD1 Healthy Lung Late Disease Lung Early Disease Lung 50 µm
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TILs are functionally impaired in the presence of tumor cells * * %IFNγ+ * * * -+-+ Ag PD-L1+ K7M2 PD-L1- 4T1 %TNF+ * * * -+-+ Ag PD-L1+ K7M2 PD-L1- 4T1 %IL-2+ * * -+-+ Ag PD-L1+ K7M2 PD-L1- 4T1
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%IFNγ+ Control PD-L1 Ab * * %TNF+ * * * Control PD-L1 Ab %IL-2+ * * * Control PD-L1 Ab A. B. C. PD-L1 blockade restores function to TILs
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Blockade of PD-1:PD-L1 significantly enhances survival in metastatic osteosarcoma model Days post implant Percent Survival P=0.0005
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30 day PD-L1 antibody treatment does not significantly improve survival compared to 15 day treatment Is immune escape occurring?
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PD-L1 antibody treatment changes inhibitory receptor expression * *
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PD-L1 antibody treated osteosarcoma is resistant to additional treatment when injected into naïve mice. PD-L1 % of Maximum *
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Combinational PD-L1 antibody treatment coupled with conventional chemotherapy The combination improves survival as compared to chemotherapy alone but is similar to PD-L1 antibody alone.
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Combinational PD-L1 antibody coupled with CTLA-4 antibody treatment improves survival
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In conclusion PD-1/PD-L1 interaction induces immune tolerance in metastatic osteosarcoma PD-L1 blockade improves survival but not 100% Resistance to therapy develops by up-regulation of alternative immune escape pathways Combinational immune therapies may have the highest impact on disease control in metastatic osteosarcoma
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Joseph Blattman Danielle Lussier John Johnson Lauren O’Neill Lizbeth Nieves Megan McAfee Susan Holechek Paul Dickman Patients and families Acknowledgements
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