| Literature DB >> 32538536 |
Stanley C Jordan1, Noriko Ammerman1, Jua Choi1, Edmund Huang1, Alice Peng1, Supreet Sethi1, Reiad Najjar1, Irene Kim1, Mieko Toyoda1, Sanjeev Kumar1, Kathlyn Lim1, Ashley Vo1.
Abstract
Modification of pathogenic antibodies and their effector functions in autoimmune diseases or use of B cell/plasma cell-directed anticancer therapies have illuminated the biologic relevance of B cells, plasma cells (PCs), and pathogenic antibodies and complement in alloimmunity. They have also rejuvenated interest in how B cells mediate multiple effector functions that include antibody production, antigen presentation to T cells, costimulation, and the production of immune stimulating and immune modulatory cytokines that drive dysfunctional immune responses. Current methods to reduce alloantibodies are only modestly successful. Rituximab is used for desensitization and antibody-mediated rejection (AMR) treatment by targeting CD20 found on B-lymphocytes. However, PCs do not express CD20, likely explaining the limited success of this approach. Intravenous immunoglobulin and plasmapheresis (PLEX) have limited success due to antibody rebound. Despite attempts to develop tolerable therapeutics for management of AMR, none, to date, have been universally accepted or obtained Food and Drug Administration approval. Lack of approved therapeutics often results in patients having a much shorter graft survival due to AMR. Repurposing drugs from autoimmunity and cancer immunotherapy has rapidly yielded important advancements in the care of AMR patients. Here we discuss emerging therapeutics aimed at prevention and treatment of AMR.Entities:
Keywords: clinical research/practice; immunosuppression/immune modulation; kidney transplantation/nephrology; rejection: antibody-mediated (ABMR); sensitization
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Year: 2020 PMID: 32538536 DOI: 10.1111/ajt.15913
Source DB: PubMed Journal: Am J Transplant ISSN: 1600-6135 Impact factor: 8.086