Ablation of B7-H3 but not B7-H4 results in highly increased tumor burden in a murine model of spontaneous prostate cancer

Katharina Kreymborg; Stefan Haak; Rajmohan Murali; Joyce Wei; Rebecca Waitz; Georg Gasteiger; Peter A. Savage; Marcel R.M. Van Den Brink; James P. Allison

Journal ArticleOPEN ACCESS

Ablation of B7-H3 but not B7-H4 results in highly increased tumor burden in a murine model of spontaneous prostate cancer

Cancer Immunology Research (2015) 3(8) 849-854

DOI: 10.1158/2326-6066.CIR-15-0100

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Abstract

The costimulatory molecules B7-H3 and B7-H4 are overexpressed in a variety of human tumors and have been hypothesized as possible biomarkers and immunotherapeutic targets. Despite this potential, the predominating uncertainty about their functional implication in tumor-host interaction hampers their evaluation as a target for cancer therapy. By means of a highly physiologic, spontaneous tumor model in mice, we establish a causal link between B7-H3 and host tumor control and found B7-H4 to be redundant.

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Kreymborg, K., Haak, S., Murali, R., Wei, J., Waitz, R., Gasteiger, G., … Allison, J. P. (2015). Ablation of B7-H3 but not B7-H4 results in highly increased tumor burden in a murine model of spontaneous prostate cancer. Cancer Immunology Research, 3(8), 849–854. https://doi.org/10.1158/2326-6066.CIR-15-0100

Ablation of B7-H3 but not B7-H4 results in highly increased tumor burden in a murine model of spontaneous prostate cancer

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