| Literature DB >> 24486575 |
Alexandre Bosch1, Santiago Llorente2, Jorge Eguia1, Anna Mrowiec1, Francisco Boix1, Ruth López-Hernández1, José A Campillo1, Gema Salgado1, Maria R Moya-Quiles1, Alfredo Minguela1, Luisa Jimeno2, María R Alvarez-López1, Manuel Muro3.
Abstract
We report an interesting case concerning an irreversible antibody-mediated rejection (AMR), associated with anti-HLA-C DSA, which occurred after a second kidney transplantation despite having determined a low number of antibodies directed against HLA-C antigens (MFI<1000) in the previous transplantation (which was then considered to be an indicator of low risk of AMR). A 63-year-old woman was re-transplanted with pre-transplant (PrT) sensitization. On day 7 post-transplantation, oligoanuria occurred and increased MFIs for the detected PrT antibodies and other antibodies (non-detected or detected with very low PrT MFI) were observed. SAB assay also showed antibodies against the second donor HLA-C mismatches and other HLA-C antigens. Nephrologists suspected AMR and the patient was therefore treated with methylprednisolone/plasmapheresis/IVIG/anti-CD20 without improvement, which led to transplantectomy. Histologic analysis confirmed acute AMR. Interestingly, it was possible to define exactly the potential immunizing epitopes whose recognition determines the specific antibody production. So, 1st donor DSAs (detected PrT with low MFI), 2nd donor DSAs (detected PTP), and non-DSA detected PTP have several shared eplets, being the 11AVR eplet the only one present on all alleles. Thus, the recognition of 11AVR eplet in the first transplant modeled the patient's antibody response. Therefore, we propose that donor HLA-C typing should always be performed for recipients with anti-HLA-C antibodies, and specific shared-eplets should be investigated in order to determine previous transplant mismatches.Entities:
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Year: 2014 PMID: 24486575 DOI: 10.1016/j.humimm.2014.01.010
Source DB: PubMed Journal: Hum Immunol ISSN: 0198-8859 Impact factor: 2.850