Inhibition of osteolytic bone metastasis of breast cancer by combined treatment with the bisphosphonate ibandronate and tissue inhibitor of the matrix metalloproteinase-2

T Yoneda, A Sasaki, C Dunstan, P J Williams, F Bauss, Y A De Clerck, G R Mundy, T Yoneda, A Sasaki, C Dunstan, P J Williams, F Bauss, Y A De Clerck, G R Mundy

Abstract

Multiple steps are involved in the metastasis of cancer cells from primary sites to distant organs. These steps should be considered in the design of pharmacologic approaches to prevent or inhibit the metastatic process. In the present study, we have compared the effects of inhibiting several steps involved in the bone metastatic process individually with inhibition of both together. The steps we chose were matrix metalloproteinase (MMP) secretion, likely involved in tumor cell invasion, and osteoclastic bone resorption, the final step in the process. We used an experimental model in which inoculation of human estrogen-independent breast cancer MDA-231 cells into the left cardiac ventricle of female nude mice causes osteolytic lesions in bone. To inhibit cancer invasiveness, the tissue inhibitor of the MMP-2 (TIMP-2), which is a natural inhibitor of MMPs, was overexpressed in MDA-231 cells. To inhibit bone resorption, a potent bisphosphonate, ibandronate (4 microg/mouse) was daily administered subcutaneously. Nude mice received either; (a) nontransfected MDA-231 cells; (b) nontransfected MDA231 cells and ibandronate; (c) TIMP-2-transfected MDA-231 cells; or (d) TIMP-2-transfected MDA-231 cells and ibandronate. In mice from group a, radiographs revealed multiple osteolytic lesions. However, in mice from group b or group c, osteolytic lesions were markedly decreased. Of particular note, in animals from group d receiving both ibandronate and TIMP-2-transfected MDA-231 cells, there were no radiologically detectable osteolytic lesions. Survival rate was increased in mice of groups c and d. There was no difference in local enlargement in the mammary fat pad between nontransfected and TIMP-2-transfected MDA-231 cells. These results suggest that inhibition of both MMPs and osteoclastic bone resorption are more efficacious treatment for prevention of osteolytic lesions than either alone, and suggest that when therapies are designed based on the uniqueness of the bone microenvironment and combined with several common steps in the metastatic process, osteolytic bone metastases can be more efficiently and selectively inhibited.

References

    1. J Morphol. 1971 Apr;133(4):417-37
    1. N Engl J Med. 1996 Dec 12;335(24):1785-91
    1. J Surg Oncol. 1979;11(3):193-205
    1. Br J Cancer. 1987 Jan;55(1):61-6
    1. Endocrinology. 1989 Mar;124(3):1539-47
    1. Cancer Res. 1990 Feb 1;50(3):717-21
    1. Cancer Res. 1990 Oct 1;50(19):6130-8
    1. J Clin Oncol. 1991 Mar;9(3):468-77
    1. Cancer Res. 1992 Feb 1;52(3):701-8
    1. Biochemistry. 1992 Feb 18;31(6):1665-72
    1. J Bone Miner Res. 1991 Sep;6(9):1003-11
    1. Bioessays. 1992 Mar;14(3):185-94
    1. Cancer Res. 1992 Oct 1;52(19):5395-9
    1. Cancer Res. 1993 Jan 1;53(1):140-6
    1. Biochem J. 1993 Jan 15;289 ( Pt 2):411-6
    1. Biochim Biophys Acta. 1993 May 8;1177(1):71-4
    1. Invasion Metastasis. 1993;13(1):31-7
    1. J Natl Cancer Inst. 1993 Nov 3;85(21):1758-64
    1. Curr Opin Cell Biol. 1993 Oct;5(5):806-11
    1. J Clin Invest. 1993 Dec;92(6):2569-76
    1. Anal Biochem. 1993 Dec;215(2):171-9
    1. Clin Exp Metastasis. 1994 Jul;12(4):305-14
    1. Cancer Res. 1994 Sep 1;54(17):4791-7
    1. Cancer Res. 1994 Oct 15;54(20):5467-73
    1. CA Cancer J Clin. 1995 Jan-Feb;45(1):8-30
    1. Breast Cancer Res Treat. 1994;32(1):73-84
    1. J Cell Sci. 1994 Sep;107 ( Pt 9):2373-9
    1. EMBO J. 1995 Mar 1;14(5):908-17
    1. Lab Invest. 1995 Mar;72(3):311-22
    1. Cancer Res. 1995 Aug 15;55(16):3551-7
    1. J Natl Cancer Inst. 1995 Oct 18;87(20):1546-50
    1. J Natl Cancer Inst. 1995 Nov 1;87(21):1588-92
    1. Int J Cancer. 1995 Dec 11;63(6):823-30
    1. Sci Am. 1996 Sep;275(3):72-7
    1. Cancer Res. 1996 Sep 1;56(17):4063-70
    1. J Cell Sci. 1995 Dec;108 ( Pt 12):3649-59
    1. J Bone Miner Res. 1996 Jan;11(1):72-8
    1. Cancer Metastasis Rev. 1995 Dec;14(4):351-62
    1. J Clin Invest. 1996 Oct 1;98(7):1544-9
    1. J Natl Cancer Inst. 1974 Sep;53(3):661-74

Source: PubMed

スポンサーと協力者

医学的状態

薬物療法

3
購読する