Literature DB >> 21033767

Optimizing therapeutic antibody function: progress with Fc domain engineering.

Etsuji Kaneko1, Rinpei Niwa.   

Abstract

Since the establishment of monoclonal antibody production using hybridoma technology in the mid-1970s, there has been expanding progress and continuous technological improvement in the development of therapeutic antibodies. The initial technological breakthroughs involved reduction of immunogenicity and thus enabled repeated administration. The establishment of chimeric, humanized, and fully human antibodies has led to the great success of several ‘second-generation’ therapeutic antibodies, such as rituximab, trastuzumab, cetuximab, and bevacizumab. However, there still exists an urgent demand for improvement in the efficacy of the current antibody therapeutics, which is not yet fully satisfactory for patients. Based on the current understanding of the clinical mechanisms of several therapeutic antibodies, many now believe that Fc-mediated functions (e.g. antibody-dependent cellular cytotoxicity, complement-dependent cytotoxicity, and neonatal Fc receptor [FcRn]-mediated storage) will improve the clinical outcomes of therapeutic antibodies. The present review focuses on the recent progress in the development of ‘Fc engineering,’ which dramatically improves (and sometimes silences) Fc-mediated functions. These achievements can be classified into two technological approaches: (i) introducing amino acid mutations and (ii) modifying Fc-linked oligosaccharide structures. The effectiveness of multiple third-generation therapeutic antibodies armed with various engineered Fcs is now ready to be tested in clinical trials.

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Year:  2011        PMID: 21033767     DOI: 10.2165/11537830-000000000-00000

Source DB:  PubMed          Journal:  BioDrugs        ISSN: 1173-8804            Impact factor:   5.807


  15 in total

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2.  Pharmacokinetics and toxicology of therapeutic proteins: Advances and challenges.

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Review 3.  One target, different effects: a comparison of distinct therapeutic antibodies against the same targets.

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Journal:  Exp Mol Med       Date:  2011-10-31       Impact factor: 8.718

Review 4.  Absorption, distribution, metabolism, and excretion (ADME) studies of biotherapeutics for autoimmune and inflammatory conditions.

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Journal:  AAPS J       Date:  2012-07-14       Impact factor: 4.009

5.  Molecular characterization and functional activity of an IL-15 antagonist MutIL-15/Fc human fusion protein.

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6.  Stabilizing the CH2 Domain of an Antibody by Engineering in an Enhanced Aromatic Sequon.

Authors:  Wentao Chen; Leopold Kong; Stephen Connelly; Julia M Dendle; Yu Liu; Ian A Wilson; Evan T Powers; Jeffery W Kelly
Journal:  ACS Chem Biol       Date:  2016-04-29       Impact factor: 5.100

7.  Aggregates, crystals, gels, and amyloids: intracellular and extracellular phenotypes at the crossroads of immunoglobulin physicochemical property and cell physiology.

Authors:  Haruki Hasegawa
Journal:  Int J Cell Biol       Date:  2013-03-05

Review 8.  Etanercept biosimilars.

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Journal:  Rheumatol Int       Date:  2014-07-01       Impact factor: 2.631

9.  Production of α2,6-sialylated IgG1 in CHO cells.

Authors:  Céline Raymond; Anna Robotham; Maureen Spearman; Michael Butler; John Kelly; Yves Durocher
Journal:  MAbs       Date:  2015       Impact factor: 5.857

10.  CF750-A33scFv-Fc-Based Optical Imaging of Subcutaneous and Orthotopic Xenografts of GPA33-Positive Colorectal Cancer in Mice.

Authors:  Danfeng Wei; Qing Fan; Huawei Cai; Hao Yang; Lin Wan; Lin Li; Xiaofeng Lu
Journal:  Biomed Res Int       Date:  2015-05-21       Impact factor: 3.411

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