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Potentiation of cytotoxic cancer therapies by TNP‐470 alone and with other anti‐angiogenic agents
Author(s) -
Teicher Beverly A.,
Holden Sylvia A.,
Ara Gulshan,
Sotomayor Enrique Alvarez,
Huang Zhen Dong,
Chen YingNan,
Brem Harold
Publication year - 1994
Publication title -
international journal of cancer
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.475
H-Index - 234
eISSN - 1097-0215
pISSN - 0020-7136
DOI - 10.1002/ijc.2910570624
Subject(s) - lewis lung carcinoma , cytotoxic t cell , in vivo , cyclophosphamide , fibrosarcoma , cancer research , medicine , cancer , lung cancer , pharmacology , immunology , pathology , chemotherapy , metastasis , in vitro , chemistry , biology , biochemistry , microbiology and biotechnology
The ability of TNP‐470, a synthetic analog of fumagillin which has been described as an anti‐angiogenic agent, to potentiate cytotoxic cancer therapies was investigated in vivo in the murine FSaIIC fibrosarcoma and the Lewis lung carcinoma. TNP‐470 was more toxic toward FSaIIC tumor cells from tumors treated in vivo than toward bone‐marrow CFU‐GM from the same animals. TNP‐470 had a dose‐modifying effect on the toxicity of cyclophosphamide toward FSaIIC tumor cells which amounted to an 8‐fold increase in tumor‐cell killing at a cyclophosphamide dose of 500 mg/kg. Treatment with TNP‐470 and minocycline increased the permeability of the FSaII fibrosarcoma in vivo to the fluorescent dye Hoechst 33342 and increased the killing of both the bright and the dim tumor cells by cyclophosphamide. TNP‐470, especially in combination with minocycline, formed a highly effective modulator combination for treatment of the Lewis lung carcinoma with cytotoxic cancer therapies against primary and metastatic disease. The combination of TNP‐470/minocycline and cyclophosphamide led to 40 to 50% long‐term survivors in Lewis‐lung‐carcinoma‐bearing animals. Our results indicate that the use of anti‐angiogenic modulators in cancer therapy is a very promising area for further study. © 1994 Wiley‐Liss, Inc.
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