Literature DB >> 8575795

Generation, characterization, and in vivo studies of humanized anticarcinoma antibody CC49.

S V Kashmiri1, L Shu, E A Padlan, D E Milenic, J Schlom, P H Hand.   

Abstract

Monoclonal antibody (MAb) CC49 reacts with tumor-associated glycoprotein (TAG)-72, a human pancarcinoma antigen. In clinical trials, radiolabeled CC49 has shown excellent tumor localization; however, many of the patients receiving MAb CC49 develop a human antimouse antibody response. In an attempt to prevent this antiimmunoglobulin response, we have developed a humanized CC49 (HuCC49) by grafting the MAb CC49 hypervariable regions onto the variable light (VL) and variable heavy (VH) frameworks of the human MAbs LEN and 21/28' CL, respectively, while retaining those murine framework residues that may be required for the integrity of the antigen combining-site structure. The HuCC49 MAb was compared with native murine CC49 (nCC49) and chimeric CC49 (cCC49), using a variety of assays. SDS-PAGE analysis under nonreducing conditions showed that the HuCC49 MAb has virtually identical mobility to that of cCC49. Under reducing conditions, the HuCC49 yielded two bands of approximately 25-28 and approximately 50-55 kDa, characteristic of heavy and light immunoglobulin chains. In competition radioimmunoassays, HuCC49 completely inhibited the binding of 125I-labeled nCC49 to TAG-72, although 23- to 30-fold more HuCC49 was required to achieve a level of competition similar to those of cCC49 and nCC49. The relative affinity of HuCC49 was 2- to 3-fold less than those of the cCC49 and nCC49 MAbs, respectively. The plasma clearance in mice of HuCC49 was virtually identical to that of cCC49. Biodistribution studies demonstrated equivalent tumor-targeting of HuCC49 and cCC49 to human colon carcinoma xenografts. These studies thus suggest that HuCC49 and genetically modified molecules, such as sFv and domain-deleted immunoglobulins developed by using the HuCC49 variable region as a cassette, may be potentially useful in both diagnostic and therapeutic clinical trials in patients with TAG-72-positive tumors.

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Year:  1995        PMID: 8575795     DOI: 10.1089/hyb.1995.14.461

Source DB:  PubMed          Journal:  Hybridoma        ISSN: 0272-457X


  12 in total

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2.  Identification of a high affinity TAG-72 binding peptide by phage display selection.

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Authors:  Lanyan Fang; Robert F Battisti; Hao Cheng; Philip Reigan; Yan Xin; Jie Shen; David Ross; Kenneth K Chan; Edward W Martin; Peng George Wang; Duxin Sun
Journal:  J Med Chem       Date:  2006-10-19       Impact factor: 7.446

4.  Development of oligoclonal nanobodies for targeting the tumor-associated glycoprotein 72 antigen.

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Journal:  Mol Biotechnol       Date:  2013-06       Impact factor: 2.695

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6.  Humanized Anti-Tumor-Associated Glycoprotein-72 for Submillimeter Near-Infrared Detection of Colon Cancer in Metastatic Mouse Models.

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Journal:  Br J Cancer       Date:  2005-04-25       Impact factor: 7.640

8.  Safety, tumor trafficking and immunogenicity of chimeric antigen receptor (CAR)-T cells specific for TAG-72 in colorectal cancer.

Authors:  Kristen M Hege; Emily K Bergsland; George A Fisher; John J Nemunaitis; Robert S Warren; James G McArthur; Andy A Lin; Jeffrey Schlom; Carl H June; Stephen A Sherwin
Journal:  J Immunother Cancer       Date:  2017-03-21       Impact factor: 13.751

9.  Humanized anti-Sialyl-Tn antibodies for the treatment of ovarian carcinoma.

Authors:  David A Eavarone; Linah Al-Alem; Alexey Lugovskoy; Jillian M Prendergast; Rawan I Nazer; Jenna N Stein; Daniel T Dransfield; Jeff Behrens; Bo R Rueda
Journal:  PLoS One       Date:  2018-07-27       Impact factor: 3.240

10.  Gamma probes and their use in tumor detection in colorectal cancer.

Authors:  Ismet Sarikaya; Ali Sarikaya; Richard C Reba
Journal:  Int Semin Surg Oncol       Date:  2008-11-19
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