In Vitro and In Vivo Induction of Antiangiogenic Activity by Plasminogen Activators and Captopril

doi:10.1093/jnci/95.5.388

JNCI Journal of the National Cancer Institute 2003 95(5):388-399; doi:10.1093/jnci/95.5.388
© 2003 by Oxford University Press

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Journal of the National Cancer Institute, Vol. 95, No. 5, 388-399, March 5, 2003
© 2003 Oxford University Press

ARTICLE

In Vitro and In Vivo Induction of Antiangiogenic Activity by Plasminogen Activators and Captopril

Jaime R. Merchan, Barden Chan, Sujata Kale, Lowell E. Schnipper, Vikas P. Sukhatme

Affiliations of authors: J. R. Merchan, Division of Hematology-Oncology, Department of Medicine and the Center for Study of the Tumor Microenvironment, Beth Israel Deaconess Medical Center and Harvard Medical School, Boston, MA, and The Clinical Investigator Training Program, Beth Israel Deaconess Medical Center–Harvard/Massachusetts Institute of Technology Health Sciences and Technology, in collaboration with Pfizer Inc.; B. Chan, S. Kale, Division of Nephrology, Department of Medicine and the Center for Study of the Tumor Microenvironment, Beth Israel Deaconess Medical Center and Harvard Medical School; L. E. Schnipper, Division of Hematology-Oncology, Department of Medicine and the Center for Study of the Tumor Microenvironment, Beth Israel Deaconess Medical Center and Harvard Medical School; V. P. Sukhatme, Divisions of Hematology-Oncology and Nephrology, Department of Medicine and the Center for Study of the Tumor Microenvironment, Beth Israel Deaconess Medical Center and Harvard Medical School.

Correspondence to: Vikas P. Sukhatme, M.D., Ph.D., Beth Israel Deaconess Medical Center, 330 Brookline Ave., Dana 517, Boston, MA 02215 (e-mail: vsukhatm{at}caregroup.harvard.edu).

Background: Many antiangiogenic molecules are proteolyticallycleaved from larger plasma proteins. For example, plasminogenactivators cleave plasminogen into plasmin, and plasmin is convertedinto angiostatin in the presence of sulfhydryl donors. We thusinvestigated whether the antiangiogenic activity in plasma couldbe increased by treatment with recombinant tissue plasminogenactivator (rt-PA) and the sulfhydryl donor captopril. Methods:Human plasma was treated with rt-PA (10 µg/mL) and/orcaptopril (1 µM). Angiogenesis was measured in vitro byhuman endothelial cell tube formation and endothelial cell proliferationand in vivo in mice with the Matrigel plug assay. Angiostatinwas removed from treated plasma by affinity chromatography,immunoprecipitation, or ion-exchange chromatography, and theantiangiogenic activity of the depleted plasma was assessedby tube formation. Three cancer patients were treated with rt-PAand captopril, and their pretreatment and post-treatment plasmaswere tested for antiangiogenic activity in vitro. Results: Angiogenesisin vitro was stimulated by untreated plasma and inhibited byplasma that had been treated with rt-PA and captopril but wasnot affected by treatment with rt-PA and/or captopril alone.In vivo angiogenesis in Matrigel plugs was substantially lowerin mice treated with rt-PA and captopril than in untreated controlmice. Antiangiogenic activity in treated plasma was largelyretained after angiostatin was removed: treated plasma inhibitedangiogenesis by 64.3% (95% confidence interval [CI] = 46.4%to 82.2%), relative to untreated plasma, and treated plasmadepleted of angiostatin by affinity chromatography or immunoprecipitationinhibited angiogenesis by 65.1% (95% CI = 53.8% to 76.4%) or63.7% (95% CI = 50.9% to 76.5%), respectively. Antiangiogenicactivity of plasma from three cancer patients was higher aftertreatment with rt-PA and captopril than before such treatment.Conclusion: Treatment with rt-PA and captopril induced antiangiogenicactivity in vitro and in vivo that appears to be independentof angiostatin.

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