Endothelial Cell-Specific Receptor Tie-2 as a Therapeutic Target

Abstract

Angiopoietin-l (Ang-l) has been suggested to function as a promoter of physiological angiogenesis. We have investigated the potential role of Ang-l in breast cancer under clinical conditions and in experimental animals. Ang-l expression in breast cancer specimens was analyzed by using laser capture micro-dissection and RT-PCR. Cancer cells adjacent to micro-vessels expressing Tie-2 were dissected and analyzed. Ang-l mRNA was detected only in 3 of 21 cases and none of 9 normal specimens. The gene was then overexpressed in a human breast cancer cell line (MCF-7) by itself or together with FGF-l, which has been shown to enhance the angiogenic phenotype and tumorigenicity of this cell line. The overexpression of Ang-l had no effect on the growth of the transfected cells in culture. When inoculated in the mammary fat pads of female nude mice, however, Ang-l overexpressing cells exhibited markedly decreased tumorigenicity, and the growth rates of their xenograft tumors were significantly slower than that of the parental cells. These data support the view that Ang-l may function physiologically to promote angiogenesis by inducing vessel maturation and stabilization, but this may inhibit angiogenesis in tumor where the vasculature is highly immature and unstable.

Document Details

Document Type

Technical Report

Publication Date

Jul 01, 2000

Accession Number

ADA388105

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