Data from Inhibition of Prostate Cancer Osteoblastic Progression with VEGF<sub>121</sub>/rGel, a Single Agent Targeting Osteoblasts, Osteoclasts, and Tumor Neovasculature

Purpose: A hallmark of prostate cancer (PCa) progression is the development of osteoblastic bone metastases, which respond poorly to available therapies. We previously reported that VEGF₁₂₁/rGel targets osteoclast precursors and tumor neovasculature. Here we tested the hypothesis that targeting nontumor cells expressing these receptors can inhibit tumor progression in a clinically relevant model of osteoblastic PCa.

Experimental Design: Cells from MDA PCa 118b, a PCa xenograft obtained from a bone metastasis in a patient with castrate-resistant PCa, were injected into the femurs of mice. Osteoblastic progression was monitored following systemic administration of VEGF₁₂₁/rGel.

Results: VEGF₁₂₁/rGel was cytotoxic in vitro to osteoblast precursor cells. This cytotoxicity was specific as VEGF₁₂₁/rGel internalization into osteoblasts was VEGF₁₂₁ receptor driven. Furthermore, VEGF₁₂₁/rGel significantly inhibited PCa-induced bone formation in a mouse calvaria culture assay. In vivo, VEGF₁₂₁/rGel significantly inhibited the osteoblastic progression of PCa cells in the femurs of nude mice. Microcomputed tomographic analysis revealed that VEGF₁₂₁/rGel restored the bone volume fraction of tumor-bearing femurs to values similar to those of the contralateral (non–tumor-bearing) femurs. VEGF₁₂₁/rGel significantly reduced the number of tumor-associated osteoclasts but did not change the numbers of peritumoral osteoblasts. Importantly, VEGF₁₂₁/rGel-treated mice had significantly less tumor burden than control mice. Our results thus indicate that VEGF₁₂₁/rGel inhibits osteoblastic tumor progression by targeting angiogenesis, osteoclastogenesis, and bone formation.

Conclusions: Targeting VEGF receptor (VEGFR)-1- or VEGFR-2–expressing cells is effective in controlling the osteoblastic progression of PCa in bone. These findings provide the basis for an effective multitargeted approach for metastatic PCa. Clin Cancer Res; 17(8); 2328–38. ©2011 AACR.