Mouse Endostatin Inhibits the Formation of Lung and Liver Metastases

Infection and Cancer: Biology, Therapeutics, and Prevention

Cancer Health Disparities Conference 2009

Tumor Biology

Mouse Endostatin Inhibits the Formation of Lung and Liver Metastases¹

Sam S. Yoon, Hiroshi Eto², Cheng-mao Lin, Hideo Nakamura, Timothy M. Pawlik, Sun U. Song and Kenneth K. Tanabe³

Division of Surgical Oncology, Department of Surgery, Massachusetts General Hospital, and Harvard Medical School, Boston, Massachusetts 02114

Angiogenesis is required for tumor formation. Several studieshave demonstrated that tumor angiogenesis is regulated by abalance between proangiogenesis and antiangiogenesis factorsand that this balance varies in different organ environments.To investigate whether expression of an angiogenesis inhibitorby cancer cells could alter this balance and prevent tumor formationin different organ environments, we engineered stable transfectantsfrom RenCa mouse renal carcinoma cells and SW620 human coloncarcinoma cells to constitutively secrete a mouse endostatinprotein with c-myc and polyhistidine (His) tags. Productionand secretion of the endostatin-c-myc-His fusion protein byendostatin-transfected cells were confirmed by immunofluorescencestaining and Western blot analysis. The endostatin transfectantsand control transfectants, stably transfected with a controlplasmid, had similar in vitro growth rates compared with theirparental cell lines. Conditioned medium from endostatin-transfectedcells inhibited human umbilical vein endothelial cell proliferationby 36–51% compared with conditioned medium from controlcells. After inoculation into mice, flank tumors from endostatin-transfectedcells were 73–91% smaller than flank tumors from controlcells after 3 weeks. Inoculation of a cell mixture containing25% endostatin-transfected cells and 75% control cells resultedin inhibition of flank tumor formation as effective as afterinoculation of 100% endostatin-transfected cells. Formationof lung metastases by RenCa endostatin-transfected cells andformation of liver metastases by SW620 endostatin-transfectedcells were dramatically inhibited compared with formation ofmetastases by control cells. These findings demonstrate thatendostatin can inhibit tumor formation in different organ environmentsand that gene delivery of endostatin into even a minority oftumor cells may be an effective strategy to prevent progressionof micrometastases to macroscopic disease.

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