Most ovarian cancer patients are diagnosed
late in progression and often experience tumor recurrence and relapses
due to drug
resistance. Surface expression of matrix
metalloprotease MMP-14 on ovarian cancer cells stimulates a
tumor-stromal signaling
pathway that promotes angiogenesis and tumor
growth. In a cohort of 92 patients, we found that MMP-14 was increased
in the
serum of women with malignant ovarian tumors.
Therefore, we investigated the preclinical efficacy of a MMP-14
monoclonal antibody
that could inhibit the migratory and invasive
properties of aggressive ovarian cancer cells in vitro. MMP-14 antibody
disrupted
ovarian tumor-stromal communication and was
equivalent to Avastin in suppressing blood vessel growth in mice
harboring matrigel
plugs. These effects on angiogenesis correlated
with down regulation of several important angiogenic factors. Further,
mice
with ovarian cancer tumors treated with anti-MMP-14
monotherapy showed a marked and sustained regression in tumor growth
with
decreased angiogenesis compared to IgG treated
controls. In a model of advanced peritoneal ovarian cancer,
MMP-14-dependent
invasion and metastasis was effectively inhibited
by intraperitoneal administration of monoclonal MMP-14 antibody.
Together,
these studies provide a preclinical
proof-of-concept for MMP-14 targeting as an adjuvant treatment strategy
for advanced ovarian
cancer.
- Received April 19, 2012.
- Revision received January 11, 2013.
- Accepted February 7, 2013.
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