Vitamin D Binding Protein-Macrophage Activating Factor (DBP-maf) Inhibits Angiogenesis and Tumor Growth in Mice

O. Kisker; Shinya Onizuka; Christian M. Becker; Michael Fannon; Evelyn Flynn; Robert J. D’Amato; Bruce R. Zetter; Judah Folkman; Rahul Ray; Narasimha Swamy; Steven Pirie‐Shepherd

doi:10.1016/s1476-5586(03)80015-5

Vitamin D Binding Protein-Macrophage Activating Factor (DBP-maf) Inhibits Angiogenesis and Tumor Growth in Mice

O. Kisker(Boston Children's Hospital), Shinya Onizuka(Nagasaki University), Christian M. Becker(Boston Children's Hospital), Michael Fannon(Boston Children's Hospital), Evelyn Flynn(Boston Children's Hospital), Robert J. D’Amato(Boston Children's Hospital), Bruce R. Zetter(Harvard University), Judah Folkman(Harvard University), Rahul Ray(Boston University), Narasimha Swamy(Brown University), Steven Pirie‐Shepherd(Boston Children's Hospital)

Neoplasia

January 1, 2003

10.1016/s1476-5586(03)80015-5

Cited by 130Open Access

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Abstract

We have isolated a selectively deglycosylated form of vitamin D binding protein (DBP-maf) generated from systemically available DBP by a human pancreatic cancer cell line. DBP-maf is antiproliferative for endothelial cells and antiangiogenic in the chorioallantoic membrane assay. DBP-maf administered daily was able to potently inhibit the growth of human pancreatic cancer in immune compromised mice (T/C=0.09). At higher doses, DBP-maf caused tumor regression. Histological examination revealed that treated tumors had a higher number of infiltrating macrophages as well as reduced microvessel density, and increased levels of apoptosis relative to untreated tumors. Taken together, these data suggest that DBP-maf is an antiangiogenic molecule that can act directly on endothelium as well as stimulate macrophages to attack both the endothelial and tumor cell compartment of a growing malignancy.

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