PLoS ONE (Oct 2010)

Generation of human antigen-specific monoclonal IgM antibodies using vaccinated "human immune system" mice.

  • Pablo D Becker,
  • Nicolas Legrand,
  • Caroline M M van Geelen,
  • Miriam Noerder,
  • Nicholas D Huntington,
  • Annick Lim,
  • Etsuko Yasuda,
  • Sean A Diehl,
  • Ferenc A Scheeren,
  • Michael Ott,
  • Kees Weijer,
  • Heiner Wedemeyer,
  • James P Di Santo,
  • Tim Beaumont,
  • Carlos A Guzman,
  • Hergen Spits

DOI
https://doi.org/10.1371/journal.pone.0013137
Journal volume & issue
Vol. 5, no. 10

Abstract

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Passive transfer of antibodies not only provides immediate short-term protection against disease, but also can be exploited as a therapeutic tool. However, the 'humanization' of murine monoclonal antibodies (mAbs) is a time-consuming and expensive process that has the inherent drawback of potentially altering antigenic specificity and/or affinity. The immortalization of human B cells represents an alternative for obtaining human mAbs, but relies on the availability of biological samples from vaccinated individuals or convalescent patients. In this work we describe a novel approach to generate fully human mAbs by combining a humanized mouse model with a new B cell immortalization technique.After transplantation with CD34+CD38⁻ human hematopoietic progenitor cells, BALB/c Rag2⁻/⁻IL-2Rγc⁻/⁻ mice acquire a human immune system and harbor B cells with a diverse IgM repertoire. "Human Immune System" mice were then immunized with two commercial vaccine antigens, tetanus toxoid and hepatitis B surface antigen. Sorted human CD19+CD27+ B cells were retrovirally transduced with the human B cell lymphoma (BCL)-6 and BCL-XL genes, and subsequently cultured in the presence of CD40-ligand and IL-21. This procedure allows generating stable B cell receptor-positive B cells that secrete immunoglobulins. We recovered stable B cell clones that produced IgM specific for tetanus toxoid and the hepatitis B surface antigen, respectively.This work provides the proof-of-concept for the usefulness of this novel method based on the immunization of humanized mice for the rapid generation of human mAbs against a wide range of antigens.