Literature DB >> 31879340

Kappa-on-Heavy (KoH) bodies are a distinct class of fully-human antibody-like therapeutic agents with antigen-binding properties.

Lynn E Macdonald1, Karoline A Meagher2, Matthew C Franklin2, Natasha Levenkova2, Johanna Hansen2, Ashok T Badithe2, Maggie Zhong2, Pamela Krueger2, Ashique Rafique2, Naxin Tu2, James Shevchuk2, Saurabh Wadhwa2, George Ehrlich2, Joannie Bautista2, Craig Grant2, Lakeisha Esau2, William T Poueymirou2, Wojtek Auerbach2, Lori Morton2, Robert Babb2, Gang Chen2, Tammy Huang2, Douglas MacDonald2, Kenneth Graham2, Cagan Gurer2, Vera A Voronina2, John R McWhirter2, Chunguang Guo2, George D Yancopoulos2, Andrew J Murphy2.   

Abstract

We describe a Kappa-on-Heavy (KoH) mouse that produces a class of highly diverse, fully human, antibody-like agents. This mouse was made by replacing the germline variable sequences of both the Ig heavy-chain (IgH) and Ig kappa (IgK) loci with the human IgK germline variable sequences, producing antibody-like molecules with an antigen binding site made up of 2 kappa variable domains. These molecules, named KoH bodies, structurally mimic naturally existing Bence-Jones light-chain dimers in their variable domains and remain wild-type in their antibody constant domains. Unlike artificially diversified, nonimmunoglobulin alternative scaffolds (e.g., DARPins), KoH bodies consist of a configuration of normal Ig scaffolds that undergo natural diversification in B cells. Monoclonal KoH bodies have properties similar to those of conventional antibodies but exhibit an enhanced ability to bind small molecules such as the endogenous cardiotonic steroid marinobufagenin (MBG) and nicotine. A comparison of crystal structures of MBG bound to a KoH Fab versus a conventional Fab showed that the KoH body has a much deeper binding pocket, allowing MBG to be held 4 Å further down into the combining site between the 2 variable domains.

Entities:  

Keywords:  alternative binding scaffolds; immunoglobulin loci; therapeutic antibodies

Mesh:

Substances:

Year:  2019        PMID: 31879340      PMCID: PMC6955234          DOI: 10.1073/pnas.1901734117

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


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