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The INNs and outs of antibody nonproprietary names

The INNs and outs of antibody nonproprietary names
The INNs and outs of antibody nonproprietary names
An important step in drug development is the assignment of an International Nonproprietary Name (INN) by the World Health Organization (WHO) that provides healthcare professionals with a unique and universally available designated name to identify each pharmaceutical substance. Monoclonal antibody INNs comprise a –mab suffix preceded by a substem indicating the antibody type, e.g., chimeric (-xi-), humanized (-zu-), or human (-u-). The WHO publishes INN definitions that specify how new monoclonal antibody therapeutics are categorized and adapts the definitions to new technologies. However, rapid progress in antibody technologies has blurred the boundaries between existing antibody categories and created a burgeoning array of new antibody formats. Thus, revising the INN system for antibodies is akin to aiming for a rapidly moving target. The WHO recently revised INN definitions for antibodies now to be based on amino acid sequence identity. These new definitions, however, are critically flawed as they are ambiguous and go against decades of scientific literature. A key concern is the imposition of an arbitrary threshold for identity against human germline antibody variable region sequences. This leads to inconsistent classification of somatically mutated human antibodies, humanized antibodies as well as antibodies derived from semi-synthetic/synthetic libraries and transgenic animals. Such sequence-based classification implies clear functional distinction between categories (e.g., immunogenicity). However, there is no scientific evidence to support this. Dialog between the WHO INN Expert Group and key stakeholders is needed to develop a new INN system for antibodies and to avoid confusion and miscommunication between researchers and clinicians prescribing antibodies.
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Vásquez, Max
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Jones, Tim D.
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Davies, Julian
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Martin, Steve
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Jones, Tim D., Carter, Paul J., Plückthun, Andreas, Vásquez, Max, Holgate, Robert G.E., Hötzel, Isidro, Popplewell, Andrew G., Parren, Paul W.H.I., Enzelberger, Markus, Rademaker, Hendrik J., Clark, Michael R., Lowe, David C., Dahiyat, Bassil I., Smith, Victoria, Lambert, John M., Wu, Herren, Reilly, Mary, Haurum, John S., Dübel, Stefan, Huston, James S., Schirrmann, Thomas, Janssen, Richard A.J., Steegmaier, Martin, Gross, Jane A., Bradbury, Andrew R.M., Burton, Dennis R., Dimitrov, Dimiter S., Chester, Kerry A., Glennie, Martin J., Davies, Julian, Walker, Adam, Martin, Steve, McCafferty, John and Baker, Matthew P. (2016) The INNs and outs of antibody nonproprietary names. mAbs, 8 (1), 1-9. (doi:10.1080/19420862.2015.1114320). (PMID:26716992)

Record type: Article

Abstract

An important step in drug development is the assignment of an International Nonproprietary Name (INN) by the World Health Organization (WHO) that provides healthcare professionals with a unique and universally available designated name to identify each pharmaceutical substance. Monoclonal antibody INNs comprise a –mab suffix preceded by a substem indicating the antibody type, e.g., chimeric (-xi-), humanized (-zu-), or human (-u-). The WHO publishes INN definitions that specify how new monoclonal antibody therapeutics are categorized and adapts the definitions to new technologies. However, rapid progress in antibody technologies has blurred the boundaries between existing antibody categories and created a burgeoning array of new antibody formats. Thus, revising the INN system for antibodies is akin to aiming for a rapidly moving target. The WHO recently revised INN definitions for antibodies now to be based on amino acid sequence identity. These new definitions, however, are critically flawed as they are ambiguous and go against decades of scientific literature. A key concern is the imposition of an arbitrary threshold for identity against human germline antibody variable region sequences. This leads to inconsistent classification of somatically mutated human antibodies, humanized antibodies as well as antibodies derived from semi-synthetic/synthetic libraries and transgenic animals. Such sequence-based classification implies clear functional distinction between categories (e.g., immunogenicity). However, there is no scientific evidence to support this. Dialog between the WHO INN Expert Group and key stakeholders is needed to develop a new INN system for antibodies and to avoid confusion and miscommunication between researchers and clinicians prescribing antibodies.

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Accepted/In Press date: 27 October 2015
e-pub ahead of print date: 30 December 2015
Published date: 2016
Organisations: Cancer Sciences

Identifiers

Local EPrints ID: 390438
URI: http://eprints.soton.ac.uk/id/eprint/390438
ISSN: 1942-0862
PURE UUID: 60b4a158-2448-4902-bec2-3a5908a0d07a

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Date deposited: 24 Mar 2016 16:36
Last modified: 14 Mar 2024 23:18

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Contributors

Author: Tim D. Jones
Author: Paul J. Carter
Author: Andreas Plückthun
Author: Max Vásquez
Author: Robert G.E. Holgate
Author: Isidro Hötzel
Author: Andrew G. Popplewell
Author: Paul W.H.I. Parren
Author: Markus Enzelberger
Author: Hendrik J. Rademaker
Author: Michael R. Clark
Author: David C. Lowe
Author: Bassil I. Dahiyat
Author: Victoria Smith
Author: John M. Lambert
Author: Herren Wu
Author: Mary Reilly
Author: John S. Haurum
Author: Stefan Dübel
Author: James S. Huston
Author: Thomas Schirrmann
Author: Richard A.J. Janssen
Author: Martin Steegmaier
Author: Jane A. Gross
Author: Andrew R.M. Bradbury
Author: Dennis R. Burton
Author: Dimiter S. Dimitrov
Author: Kerry A. Chester
Author: Julian Davies
Author: Adam Walker
Author: Steve Martin
Author: John McCafferty
Author: Matthew P. Baker

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