Differential effect of bortezomib on HLA class i and class II antibody

Mary Carmelle Philogene, Paul Sikorski, Robert A. Montgomery, Mary S. Leffell, Andrea A. Zachary

Research output: Contribution to journalArticlepeer-review

27 Scopus citations

Abstract

BACKGROUND: Bortezomib has been used to reduce HLA antibody in patients either before transplantation or as treatment for antibody-mediated rejection (AMR). Reports on its efficacy show mixed results. The mechanism of action of this agent is via proteasome inhibition. The primary route of synthesis of HLA class I molecules is dependent on peptide generation by the proteasome, whereas that of class II is not. We observed a differential effect of bortezomib on class I versus class II antibody and hypothesized that this was related to a reduced expression of class I HLA antigens. METHODS: The effect of bortezomib on HLA antibody levels was evaluated in 13 patients who were desensitized for incompatible renal transplantation. We calculated the percent difference in HLA antibody level before and after bortezomib treatment and the impact of bortezomib on HLA expression in lymphocytes of healthy control subjects. RESULTS: On average, the level of HLA class I donor-specific antibody (DSA) decreased by 32%, whereas that of class II DSA increased by 29%. In vitro bortezomib treatment of lymphocytes resulted in a mean decrease of 23% in MHC class I expression on B lymphocytes and no change (+1.08%) in MHC class II expression (P=0.0003). The amount of intracellular class I molecules was reduced by a mean of 29% with bortezomib. CONCLUSION: These data indicate that bortezomib reduces HLA class I antibody more effectively than class II antibody. This difference may be due to the reduced expression of class I molecules resulting from treatment with this proteasome inhibitor.

Original languageEnglish (US)
Pages (from-to)660-665
Number of pages6
JournalTransplantation
Volume98
Issue number6
DOIs
StatePublished - Sep 27 2014

Keywords

  • Bortezomib
  • HLA antibody
  • MHC molecules
  • Proteasome inhibition
  • Renal transplantation

ASJC Scopus subject areas

  • Transplantation

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