Literature DB >> 18474866

Comprehensive screening for antigens overexpressed on carcinomas via isolation of human mAbs that may be therapeutic.

Gene Kurosawa1, Yasushi Akahori, Miwa Morita, Mariko Sumitomo, Noriko Sato, Chiho Muramatsu, Keiko Eguchi, Kazuki Matsuda, Akihiko Takasaki, Miho Tanaka, Yoshitaka Iba, Susumu Hamada-Tsutsumi, Yoshinori Ukai, Mamoru Shiraishi, Kazuhiro Suzuki, Maiko Kurosawa, Sally Fujiyama, Nobuhiro Takahashi, Ryoichi Kato, Yoshikazu Mizoguchi, Mikihiro Shamoto, Hiroyuki Tsuda, Mototaka Sugiura, Yoshinobu Hattori, Shuichi Miyakawa, Ryoichi Shiroki, Kiyotaka Hoshinaga, Nobuhiro Hayashi, Atsushi Sugioka, Yoshikazu Kurosawa.   

Abstract

Although several murine mAbs that have been humanized became useful therapeutic agents against a few malignancies, therapeutic Abs are not yet available for the majority of the human cancers because of our lack of knowledge of which antigens (Ags) can become useful targets. In the present study we established a procedure for comprehensive identification of such Ags through the extensive isolation of human mAbs that may become therapeutic. Using the phage-display Ab library we isolated a large number of human mAbs that bind to the surface of tumor cells. They were individually screened by immunostaining, and clones that preferentially and strongly stained the malignant cells were chosen. The Ags recognized by those clones were isolated by immunoprecipitation and identified by MS. We isolated 2,114 mAbs with unique sequences and identified 21 distinct Ags highly expressed on several carcinomas. Of those 2,114 mAbs 356 bound specifically to one of the 21 Ags. After preparing complete IgG(1) Abs the in vitro assay for Ab-dependent cell-mediated cytotoxicity (ADCC) and the in vivo assay in cancer-bearing athymic mice were performed to examine antitumor activity. The mAbs converted to IgG(1) revealed effective ADCC as well as antitumor activity in vivo. Because half of the 21 Ags showed distinct tumor-specific expression pattern and the mAbs isolated showed various characteristics with strong affinity to the Ag, it is likely that some of the Ags detected will become useful targets for the corresponding carcinoma therapy and that several mAbs will become therapeutic agents.

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Year:  2008        PMID: 18474866      PMCID: PMC2377314          DOI: 10.1073/pnas.0712202105

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  22 in total

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Journal:  Cancer Res       Date:  2001-03-01       Impact factor: 12.701

6.  Humanization of an anti-p185HER2 antibody for human cancer therapy.

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7.  Identification and characterization of tumor antigens by using antibody phage display and intrabody strategies.

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10.  Proteomic analysis of integral plasma membrane proteins.

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  30 in total

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Journal:  Arch Biochem Biophys       Date:  2012-05-22       Impact factor: 4.013

2.  ICAM-1 targeting of doxorubicin-loaded PLGA nanoparticles to lung epithelial cells.

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3.  A 3D matrix platform for the rapid generation of therapeutic anti-human carcinoma monoclonal antibodies.

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Review 4.  Selection strategies for anticancer antibody discovery: searching off the beaten path.

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Review 5.  Ligandomics: a paradigm shift in biological drug discovery.

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6.  Antibody library screens using detergent-solubilized mammalian cell lysates as antigen sources.

Authors:  Yong Ku Cho; Eric V Shusta
Journal:  Protein Eng Des Sel       Date:  2010-05-23       Impact factor: 1.650

Review 7.  Principles of early drug discovery.

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9.  Comprehensive Identification of Tumor-associated Antigens via Isolation of Human Monoclonal Antibodies that may be Therapeutic.

Authors:  Yoshikazu Kurosawa
Journal:  Immune Netw       Date:  2009-02-28       Impact factor: 6.303

10.  Evaluation of (89)Zr-labeled human anti-CD147 monoclonal antibody as a positron emission tomography probe in a mouse model of pancreatic cancer.

Authors:  Aya Sugyo; Atsushi B Tsuji; Hitomi Sudo; Kotaro Nagatsu; Mitsuru Koizumi; Yoshinori Ukai; Gene Kurosawa; Ming-Rong Zhang; Yoshikazu Kurosawa; Tsuneo Saga
Journal:  PLoS One       Date:  2013-04-05       Impact factor: 3.240

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