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Summary
November 2006, Vol. 6, No. 11, Pages 1161-1173
, DOI 10.1517/14712598.6.11.1161
Non-fucosylated therapeutic antibodies as next-generation therapeutic antibodiesMitsuo Satoh1Kyowa Hakko Kogyo Co. Ltd, Tokyo Research Laboratories, 3-6-6 Asahi-machi, Machida-shi, Tokyo 194-8533, Japan. msatoh@kyowa.co.jp †  Author for correspondenceMost of the existing therapeutic antibodies that have been licensed and developed as medical agents are of the human IgG1 isotype, the molecular weight of which is Forward Links to Citing ArticlesTsuguo Kubota, Rinpei Niwa, Mitsuo Satoh, Shiro Akinaga, Kenya Shitara, Nobuo Hanai. (2009) Engineered therapeutic antibodies with improved effector functions. Cancer Science Online publication date: 1-Jul-2009. CrossRef Stephen T Holgate. (2009) Novel targets of therapy in asthma. Current Opinion in Pulmonary Medicine 15:1, 63-71 Online publication date: 1-Feb-2009. CrossRef S. Thobhani, C.-T. Yuen, M. J A Bailey, C. Jones. (2008) Identification and quantification of N-linked oligosaccharides released from glycoproteins: An inter-laboratory study. Glycobiology 19:3, 201-211 Online publication date: 12-Dec-2008. CrossRef M. Shibata-Koyama, S. Iida, A. Okazaki, K. Mori, K. Kitajima-Miyama, S. Saitou, S. Kakita, Y. Kanda, K. Shitara, K. Kato, M. Satoh. (2008) The N-linked oligosaccharide at Fc RIIIa Asn-45: an inhibitory element for high Fc RIIIa binding affinity to IgG glycoforms lacking core fucosylation. Glycobiology 19:2, 126-134 Online publication date: 24-Nov-2008. CrossRef Sigrid R. Ruuls, Jeroen J. Lammerts van Bueren, Jan G. J. van de Winkel, Paul W. H. I. Parren. (2008) Novel human antibody therapeutics: The age of the Umabs. Biotechnology Journal 3:9-10, 1157-1171 Online publication date: 1-Nov-2008. CrossRef Johannes Stadlmann, Martin Pabst, Daniel Kolarich, Renate Kunert, Friedrich Altmann. (2008) Analysis of immunoglobulin glycosylation by LC-ESI-MS of glycopeptides and oligosaccharides. PROTEOMICS 8:14, 2858-2871 Online publication date: 1-Aug-2008. CrossRef Stephen T. Holgate, Riccardo Polosa. (2008) Treatment strategies for allergy and asthma. Nature Reviews Immunology 8:3, 218-230 Online publication date: 1-Apr-2008. CrossRef Yoshiki Yamaguchi. (2008) Trends in Glycoscience and Glycotechnology 20:112, 117-130 Online publication date: 1-Feb-2008. CrossRef Jan ter Meulen. (2007) Monoclonal antibodies for prophylaxis and therapy of infectious diseases. Expert Opinion on Emerging Drugs 12:4, 525-540 Online publication date: 1-Nov-2007. Summary | Full Text | PDF (174 KB) | PDF Plus (291 KB) Roy Jefferis. (2007) Antibody therapeutics:. Expert Opinion on Biological Therapy 7:9, 1401-1413 Online publication date: 1-Sep-2007. Summary | Full Text | PDF (641 KB) | PDF Plus (799 KB) Users who read this article also read:
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150 kDa. Human IgG1 is a glycoprotein bearing two N-linked biantennary complex-type oligosaccharides bound to the antibody constant region (Fc), in which the majority of the oligosaccharides are core fucosylated, and it exercises the effector functions of antibody-dependent cellular cytotoxicity (ADCC) and complement-dependent cytotoxicity through the interaction of the Fc with either leukocyte receptors (FcγRs) or complement. Recently, therapeutic antibodies have been shown to improve overall survival as well as time to disease progression in a variety of human malignancies, such as breast, colon and haematological cancers, and genetic analysis of FcγR polymorphisms of cancer patients has demonstrated that ADCC is a major antineoplasm mechanism responsible for clinical efficacy. However, the ADCC of existing licensed therapeutic antibodies has been found to be strongly inhibited by serum due to nonnpecific IgG competing for binding of the therapeutics to FcγRIIIa on natural killer cells, which leads to the requirement of a significant amount of drug and very high costs associated with such therapies. Moreover, enhanced ADCC of non-fucosylated forms of therapeutic antibodies through improved FcγRIIIa binding is shown to be inhibited by the fucosylated counterparts. In fact, non-fucosylated therapeutic antibodies, not including the fucosylated forms, exhibit the strongest and most saturable in vitro and ex vivo ADCC among such antibody variants with improved FcγRIIIa binding as those bearing naturally occurring oligosaccharide heterogeneities and artificial amino acid mutations, even in the presence of plasma IgG. Robust stable production of completely non-fucosylated therapeutic antibodies in a fixed quality has been achieved by the generation of a unique host cell line, in which the endogenous α-1,6-fucosyltransferase (FUT8) gene is knocked out. Thus, the application of non-fucosylated antibodies is expected to be a promising approach as next-generation therapeutic antibodies with improved efficacy, even when administrated at low doses in humans in vivo. Clinical trials using non-fucosylated antibody therapeutics are underway at present.
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