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CR011, a fully human monoclonal antibody-auristatin E conjugate, for the treatment of melanoma.

Kam Fai Tse, Michael Jeffers, Vincent A Pollack, Denise A McCabe, Melanie L Shadish, Nikolai V Khramtsov, Craig S Hackett, Suresh G Shenoy, Bing Kuang, Ferenc L Boldog, John R MacDougall, Luca Rastelli, John Herrmann, Michael Gallo, Gadi Gazit-Bornstein, Peter D Senter, Damon L Meyer, Henri S Lichenstein and William J LaRochelle
Kam Fai Tse
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Michael Jeffers
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Vincent A Pollack
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Denise A McCabe
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Melanie L Shadish
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Nikolai V Khramtsov
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Craig S Hackett
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Suresh G Shenoy
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Bing Kuang
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Ferenc L Boldog
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John R MacDougall
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Luca Rastelli
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John Herrmann
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Michael Gallo
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Gadi Gazit-Bornstein
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Peter D Senter
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Damon L Meyer
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Henri S Lichenstein
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William J LaRochelle
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DOI: 10.1158/1078-0432.CCR-05-2018 Published February 2006
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Abstract

PURPOSE: Advanced melanoma is a highly drug-refractory neoplasm representing a significant unmet medical need. We sought to identify melanoma-associated cell surface molecules and to develop as well as preclinically test immunotherapeutic reagents designed to exploit such targets. EXPERIMENTAL DESIGN AND RESULTS: By transcript profiling, we identified glycoprotein NMB (GPNMB) as a gene that is expressed by most metastatic melanoma samples examined. GPNMB is predicted to be a transmembrane protein, thus making it a potential immunotherapeutic target in the treatment of this disease. A fully human monoclonal antibody, designated CR011, was generated to the extracellular domain of GPNMB and characterized for growth-inhibitory activity against melanoma. The CR011 monoclonal antibody showed surface staining of most melanoma cell lines by flow cytometry and reacted with a majority of metastatic melanoma specimens by immunohistochemistry. CR011 alone did not inhibit the growth of melanoma cells. However, when linked to the cytotoxic agent monomethylauristatin E (MMAE) to generate the CR011-vcMMAE antibody-drug conjugate, this reagent now potently and specifically inhibited the growth of GPNMB-positive melanoma cells in vitro. Ectopic overexpression and small interfering RNA transfection studies showed that GPNMB expression is both necessary and sufficient for sensitivity to low concentrations of CR011-vcMMAE. In a melanoma xenograft model, CR011-vcMMAE induced significant dose-proportional antitumor effects, including complete regressions, at doses as low as 1.25 mg/kg. CONCLUSION: These preclinical results support the continued evaluation of CR011-vcMMAE for the treatment of melanoma.

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Clinical Cancer Research: 12 (4)
February 2006
Volume 12, Issue 4
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CR011, a fully human monoclonal antibody-auristatin E conjugate, for the treatment of melanoma.
Kam Fai Tse, Michael Jeffers, Vincent A Pollack, Denise A McCabe, Melanie L Shadish, Nikolai V Khramtsov, Craig S Hackett, Suresh G Shenoy, Bing Kuang, Ferenc L Boldog, John R MacDougall, Luca Rastelli, John Herrmann, Michael Gallo, Gadi Gazit-Bornstein, Peter D Senter, Damon L Meyer, Henri S Lichenstein and William J LaRochelle
Clin Cancer Res February 15 2006 (12) (4) 1373-1382; DOI: 10.1158/1078-0432.CCR-05-2018

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CR011, a fully human monoclonal antibody-auristatin E conjugate, for the treatment of melanoma.
Kam Fai Tse, Michael Jeffers, Vincent A Pollack, Denise A McCabe, Melanie L Shadish, Nikolai V Khramtsov, Craig S Hackett, Suresh G Shenoy, Bing Kuang, Ferenc L Boldog, John R MacDougall, Luca Rastelli, John Herrmann, Michael Gallo, Gadi Gazit-Bornstein, Peter D Senter, Damon L Meyer, Henri S Lichenstein and William J LaRochelle
Clin Cancer Res February 15 2006 (12) (4) 1373-1382; DOI: 10.1158/1078-0432.CCR-05-2018
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Clinical Cancer Research
eISSN: 1557-3265
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