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PD-1 blockade and OX40 triggering synergistically protects against tumor growth in a murine model of ovarian cancer

PLOSONE. 2014-02; 
Zhiqiang Guo , Xin Wang, Dali Cheng, Zhijun Xia, Meng Luan, Shulan Zhang
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Biochemicals … Isolated splenocytes from treated mice were cultured in the presence of 10 µg/mL H-2Db-restricted mesothelin-derived peptides (amino acid 406-414) or control HPV-E7-derived peptide (amino acid 49-57; all from GenScript, Nanjing, CA) for 3 days … Get A Quote

摘要

The co-inhibitory receptor Programmed Death-1 (PD-1) curtails immune responses and prevent autoimmunity, however, tumors exploit this pathway to escape from immune destruction. The co-stimulatory receptor OX40 is upregulated on T cells following activation and increases their clonal expansion, survival and cytokine production when engaged. Although antagonistic anti-PD-1 or agonistic anti-OX40 antibodies can promote the rejection of several murine tumors, some poorly immunogenic tumors were refractory to this treatment. In the present study, we evaluated the antitumor effects and mechanisms of combinatorial PD-1 blockade and OX40 triggering in a murine ID8 ovarian cancer model. Although individual anti-PD-1 or ... More

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