• Discovery medicine · Apr 2012

    Review Case Reports

    Evolving paradigms for desensitization in managing broadly HLA sensitized transplant candidates.

    • Nancy L Reinsmoen, Chi-Hung Lai, Ashley Vo, and Stanley C Jordan.
    • Comprehensive Transplant Center and HLA Laboratory, Cedars-Sinai Medical Center, Los Angeles, California 90048, USA. nancy.reinsmoen@cshs.org
    • Discov Med. 2012 Apr 1;13(71):267-73.

    AbstractThe broadly human leukocyte antigen (HLA) sensitized patient awaiting organ transplantation remains a persistent and significant problem for transplant medicine. Sensitization occurs as a consequence of exposure to HLA antigens through pregnancy, blood and platelet transfusions, and previous transplants. Early experience with desensitization protocols coupled with improved diagnostics for donor-specific antibodies (DSAs) and renal pathology have greatly improved transplant rates and outcomes for patients once considered un-transplantable or at high risk for poor outcomes. More recent advances have occurred through implementation of a national allocation system requiring the entering of unacceptable antigens that reduces the rate of crossmatch positivity. Current desensitization therapies include high-dose intravenous immunoglobulin (IVIG), plasma exchange (PLEX) with low-dose IVIG, and IVIG combined with rituximab. Developing therapies include proteasome inhibitors aimed at plasma cells and modifiers of complement-mediated injury. Here we discuss the important advancements in desensitization including defining the risk for antibody-mediated rejection prior to transplantation and the evolution of therapies aimed at reducing the impact of antibody injury on allografts.

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