Combination of Hedgehog Inhibitors and Standard Anticancer Agents Synergistically Prevent Osteosarcoma Growth

Overview

Journal Int J Oncol

Specialty Oncology

Date 2015 Nov 10

PMID 26548578

Citations 14

Authors

Yoshinobu Saitoh

Takao Setoguchi

Masahito Nagata

Arisa Tsuru

Shunsuke Nakamura

Satoshi Nagano

Yasuhiro Ishidou

Hiroko Nagao-Kitamoto

Masahiro Yokouchi

Shingo Maeda

Akihide Tanimoto

Tatsuhiko Furukawa

Setsuro Komiya

Affiliations

Soon will be listed here.

Abstract

High-dose chemotherapy and surgical intervention have improved long-term prognosis for non-metastatic osteosarcoma to 50-80%. However, metastatic osteosarcoma exhibits resistance to standard chemotherapy. We and others have investigated the function of Hedgehog pathway in osteosarcoma. To apply our previous findings in clinical settings, we examined the effects of Hedgehog inhibitors including arsenic trioxide (ATO) and vismodegib combined with standard anticancer agents. We performed WST-1 assays using ATO, cisplatin (CDDP), ifosfamide (IFO), doxorubicin (DOX), and vismodegib. Combination-index (CI) was used to examine synergism using CalcuSyn software. Xenograft models were used to examine the synergism in vivo. WST-1 assays showed that 143B and Saos2 cell proliferation was inhibited by ATO combined with CDDP, IFO, DOX, and vismodegib. Combination of ATO and CDDP, IFO, DOX or vismodegib was synergistic when the two compounds were used on proliferating 143B and Saos2 human osteosarcoma cells. An osteosarcoma xenograft model showed that treatment with ATO and CDDP, IFO, or vismodegib significantly prevented osteosarcoma growth in vivo compared with vehicle treatment. Our findings indicate that combination of Hedgehog pathway inhibitors and standard FDA-approved anticancer agents with established safety for human use may be an attractive therapeutic method for treating osteosarcoma.

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