1. Academic Validation
  2. An antidote approach to reduce risk and broaden utility of antibody-based therapeutics

An antidote approach to reduce risk and broaden utility of antibody-based therapeutics

  • J Biol Chem. 2017 May 19;292(20):8498-8506. doi: 10.1074/jbc.M117.775528.
Alyse D Portnoff 1 Cuihua Gao 1 M Jack Borrok 1 Xizhe Gao 2 Changshou Gao 3 G Jonah Rainey 4
Affiliations

Affiliations

  • 1 Departments of Antibody Discovery and Protein Engineering.
  • 2 Translational Sciences, MedImmune, Gaithersburg, Maryland 20878.
  • 3 Departments of Antibody Discovery and Protein Engineering. Electronic address: gaoc@medimmune.com.
  • 4 Departments of Antibody Discovery and Protein Engineering. Electronic address: jrainey@mabvax.com.
Abstract

Antibody therapeutics offer effective treatment options for a broad range of diseases. One of the greatest benefits of antibody therapeutics is their extraordinarily long serum half-life, allowing infrequent dosing with long-lasting effects. A characteristic of Antibodies that drives long half-life is the ability to interact with the recycling receptor, FcRn, in a pH-dependent manner. The benefit of long half-life, however, carries with it liabilities. Although the positive effects of antibody therapeutics are long-lasting, any acute adverse events or chronic negative impacts, such as immunosuppression in the face of an Infection, are also long-lasting. Therefore, we sought to develop Antibodies with a chemical handle that alone would enjoy the long half-life of normal Antibodies but, upon addition of a small-molecule antidote, would interact with the chemical handle and inhibit the antibody recycling mechanism, thus leading to rapid degradation and shortened half-life in vivo Here we present a proof of concept study where we identify sites to incorporate a non-natural amino acid that can be chemically modified to modulate FcRn interaction in vitro and antibody half-life in vivo This is an important first step in developing safer therapeutics, and the next step will be development of technology that can perform the modifying chemistry in vivo.

Keywords

Fc receptor; antibody engineering; biotechnology; chemical biology; drug metabolism; immunoglobulin G (IgG); monoclonal antibody; pharmacokinetics; receptor recycling.

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