A Fully Human Antitumor ImmunoRNase Selective for ErbB-2-Positive Carcinomas

doi:10.1158/0008-5472.CAN-03-3717

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[Cancer Research 64, 4870-4874, July 15, 2004]
© 2004 American Association for Cancer Research

Regular Articles

A Fully Human Antitumor ImmunoRNase Selective for ErbB-2-Positive Carcinomas

Claudia De Lorenzo¹, Angela Arciello¹, Rosanna Cozzolino¹, Donald B. Palmer², Paolo Laccetti¹, Renata Piccoli¹ and Giuseppe D’Alessio¹

¹ Department of Biological Chemistry, University of Naples Federico II, Naples, Italy, and ² Department of Veterinary Basic Sciences, The Royal Veterinary College, University of London, London, United Kingdom

We report the preparation and characterization of a novel, fullyhuman antitumor immunoRNase (IR). The IR, a human RNase andfusion protein made up of a human single chain variable fragment(scFv), is directed to the ErbB-2 receptor and overexpressedin many carcinomas. The anti-ErbB-2 IR, named hERB-hRNase, retainsthe enzymatic activity of the wild-type enzyme (human pancreaticRNase) and specifically binds to ErbB-2-positive cells withthe high affinity (K_d = 4.5 nM) of the parental scFv. hERB-hRNasebehaves as an immunoprotoxin and on internalization by targetcells becomes selectively cytotoxic in a dose-dependent mannerat nanomolar concentrations. Administered in five doses of 1.5mg/kg to mice bearing an ErbB-2-positive tumor, hERB-hRNaseinduced a dramatic reduction in tumor volume. hERB-hRNase isthe first fully human antitumor IR produced thus far, with ahigh potential as a poorly immunogenic human drug devoid ofnonspecific toxicity, directed against ErbB-2-positive malignancies.

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