Human monoclonal antibody GNX-8 directed to extended type 1 chain: Specific binding to human colorectal cancer
| Autor: | Kazuko Handa, Sen-itiroh Hakomori, Isao Ishida, Mei-Chun Yang, Feng-Lin Hsu, Jerry Ting, Liahng-Yirn Liu, Jaw-Yuan Wen, Tong-Hsuan Chang, Mei-Hsien Lee, Shu-Yen Chang |
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| Rok vydání: | 2009 |
| Předmět: |
Antibody-dependent cell-mediated cytotoxicity
Cancer Research biology medicine.drug_class business.industry medicine.medical_treatment Cancer Immunotherapy medicine.disease Monoclonal antibody Molecular biology Epitope Oncology Antigen Cell culture Immunology medicine biology.protein Antibody business |
| Zdroj: | International journal of cancer. |
| ISSN: | 1097-0215 |
| Popis: | We observed previously that two carbohydrate epitopes, extended type 1 chain Le(a)-Le(a) and Le(b)-Le(a), are expressed strongly in human gastric or colorectal cancer and cell lines derived therefrom, but their expression in human normal colorectal cells is highly limited. A monoclonal antibody, termed GNX-8, was established through immunization of "KM mice" with colonic cancer cell line Colo205, and with purified Le(b)-Le(a) glycosphingolipid, followed by screening human IgG directed to this antigen. KM mice possess human chromosome fragments and are capable of producing human immunoglobulin. GNX-8 reacted specifically with extended type 1 chain epitope Le(b)-Le(a), bound to all five colonic cancer cell lines so far tested, and displayed strong complement-dependent cytotoxicity (CDC) and antibody-dependent cellular cytotoxicity (ADCC). The antigens defined by GNX-8, expressed in Colo205 cells, were: (i) glycosphingolipids with epitope Le(b)-Le(a), whose reactivity was abolished upon defucosylation; (ii) glycoproteins with molecular mass range from 32 to >175 kDa, which were depleted in cells cultured in the presence of benzyl-alpha-GalNAc, indicating that these epitopes are O-linked glycans.Immunohistological reactivity of GNX-8 at 1 mug/ml, applied on tissue sections from colorectal and various other types of cancer, was much stronger than that with various normal cells and tissues. GNX-8 reactivity with normal cells required a much higher concentration (150 mug/ml), and this reactivity was based on cross-reaction with non-extended, normal blood group Le(b) antigen. Growth of subcutaneous xenograft of human colonic cancer cells, Colo205 or DLD-1, in nude mice or SCID mice, was strongly inhibited by administration of GNX-8. These observations, taken together, indicate that antibody GNX-8, directed specifically to Le(b)-Le(a) antigen, provides a novel direction of immunotherapy for human colorectal cancer. (c) 2009 UICC. |
| Databáze: | OpenAIRE |
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