AI Article Synopsis

  • Anti-CD2 therapy shows promise in modulating the immune system for transplant rejection, but its effectiveness is affected by species differences in the CD2 antigen.
  • A study with cynomolgus macaques tested two versions of the same anti-CD2 monoclonal antibody, finding that it significantly depleted memory T cells while sparing naive T cells and regulatory T cells (Tregs).
  • The treatment exhibited a strong inhibitory effect on mixed lymphocyte reactions and had a good safety profile, with no major adverse events, indicating its potential for future translation into clinical trials.

Article Abstract

Anti-CD2 treatment provides targeted immunomodulatory properties that have demonstrated clinical usefulness to condition the immune system and to treat transplant rejection. The treatment is species-specific due to structural CD2 antigen differences between nonhuman primates and humans. Herein, we report the safety profile and efficacy of two modifications of the same anti-CD2 monoclonal antibody in cynomolgus macaques. Twelve subjects received one i.v. anti-CD2 (of rat or rhesus type) dose each, range 1-4 mg/kg, and were followed for 1-7 days. Treatment effects were evaluated with flow cytometry on peripheral blood and histopathological evaluation of secondary lymphoid organs. In vitro inhibitory activity on primary MHC disparate mixed lymphocyte reactions (MLRs) was determined. Upon anti-CD2 treatment, CD4 , CD8 memory subsets were substantially depleted. Naïve T cells and Tregs were relatively spared and exhibited lower CD2 expression than memory T cells. Early immune reconstitution was noted for naïve cells, while memory counts had not recovered after one week. Both antibodies displayed a concentration-dependent MLR inhibition. Lymph node examination revealed no significant lymphocyte depletion. None of the animals experienced any significant study drug-related adverse events. This study outlines the safety and pharmacodynamic profile of primate-specific anti-CD2 treatment, relevant for translation of anti-CD2-based animal models into clinical trials.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7017722PMC
http://dx.doi.org/10.1111/tri.13524DOI Listing

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