Teriparatide Does Not Exacerbate Bone Metastases in Breast Cancer Bone Metastasis Model.

特立帕肽不会加剧乳腺癌骨转移模型中的骨转移

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作者:Kawaragi Takashi, Tsuchie Hiroyuki, Nagasawa Hiroyuki, Hongo Michio, Kasukawa Yuji, Nozaka Koji, Kasama Fumihito, Oya Keita, Watanabe Manabu, Tominaga Kenta, Miyakoshi Naohisa
BACKGROUND/AIM: Breast cancer frequently metastasizes to bone, and chemotherapy and hormone therapy can increase osteoporosis risk. Teriparatide (TPTD), an osteoporosis treatment that promotes bone formation, is contraindicated in patients with bone metastases due to concerns about osteosarcoma in animal studies. However, its effects on metastatic bone tumors remain unclear. This study aimed to evaluate TPTD's effects on breast cancer bone metastases using a mouse model. MATERIALS AND METHODS: C57BL/6 mice were injected with E0771 breast cancer cells to establish bone metastasis and breast cancer models. Mice were assigned to the vehicle-treated group (control) or to the TPTD-treated group (80 μg/kg, subcutaneously three times weekly). Tumor weight, volume, bone destruction, pathological fractures, distant metastasis, tumor proliferation (Ki-67, BrdU), and bone microstructure were assessed at 4 and 6 weeks. RESULTS: In both models, no significant differences in tumor weight or volume were observed between the TPTD and control groups. In the bone metastasis model, bone destruction and pathological fractures were not significantly different. No distant metastasis was observed and there were no significant differences in the percentages of Ki-67-positive and BrdU-positive cells in both models. In the bone microstructure analysis at 6 weeks post-injection, bone volume/tissue volume and trabecular thickness increased in the bone metastasis model in the TPTD group (p=0.02 and p<0.01, respectively), and trabecular separation decreased in the TPTD group (p=0.01). CONCLUSION: TPTD did not cause tumor growth, pathological fractures, or bone destruction in our in vivo models, indicating that it may be safe for use in breast cancer.

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