Antibody Fragments Humanization: Beginning with the End in Mind.

Methods Mol Biol

School of Pharmacy, Paris-Sud University, Châtenay-Malabry, France.

Published: June 2019

AI Article Synopsis

  • Molecular engineering allows the creation of smaller antibody formats like scFvs and Fabs, which have potential in living organisms but often come from rodent sources and can trigger immune responses in humans.
  • There is currently no established method to develop humanized antibody V-domains that maintain the binding ability and stability of the original rodent antibodies.
  • A proposed strategy involves grafting specific regions (CDRs) from rodent antibodies onto selected human antibody frameworks, supplemented with a flowchart for processing and a series of selection steps to identify the best humanized candidates.

Article Abstract

Molecular engineering has made possible to reformat monoclonal antibodies into smaller antigen-binding structures like scFvs, diabodies, Fabs with new potential in vivo applications because they do not induce Fc-mediated functions. However, most of these molecules are from rodent origin. As a consequence, they are immunogenic and approval for administration to humans requires prior humanization. Today, there is no well-identified strategy to create recombinant humanized antibody V-domains that preserve the antigen-binding characteristics of the parental antibody associated with high stability and solubility. Here, we propose a strategy that consists in grafting CDRs onto properly chosen human antibody frameworks in order to reduce immunogenicity. A flowchart indicates the way to proceed in order to introduce an internal affinity purification tag while structural refinements are proposed to maintain antigen-binding characteristics. The best humanized candidates are identified through selection steps including in silico analysis, research scale production followed by early functional evaluation, purification assays, aggregation, and stability assessment.

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Source
http://dx.doi.org/10.1007/978-1-4939-8958-4_10DOI Listing

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