Alloantibodies and the Outcome of Cadaver Kidney Allografts

The role of humoral immunity in causing antibody-mediated rejection (AMR) of organ allografts has been extensively documented. For this reason, negative complement-dependent cytotoxicity (CDC) cross-matches between recipient sera and donor T and B lymphocytes have become a mandatory requirement for...

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Published in:Human Immunology 2006-08, Vol.67 (8), p.597-604
Main Authors: Vasilescu, Elena Rodica, Ho, Eric K., Colovai, Adriana I., Vlad, George, Foca-Rodi, Aurica, Markowitz, Glen S., D’Agati, Vivette, Hardy, Mark A., Ratner, Lloyd E., Suciu-Foca, Nicole
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Language:English
Subjects:
antibody mediated rejection
antiHLA antibodies
C4d deposition
Cadaver
Female
flow cytometry cross-matches
Graft Rejection - immunology
Humans
Isoantibodies - blood
Kidney Transplantation - immunology
Male
Tissue Donors
Transplantation, Homologous - immunology
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creator Vasilescu, Elena Rodica
Ho, Eric K.
Colovai, Adriana I.
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Hardy, Mark A.
Ratner, Lloyd E.
Suciu-Foca, Nicole
description The role of humoral immunity in causing antibody-mediated rejection (AMR) of organ allografts has been extensively documented. For this reason, negative complement-dependent cytotoxicity (CDC) cross-matches between recipient sera and donor T and B lymphocytes have become a mandatory requirement for cadaveric kidney transplantation. However, the significance of donor-specific antibodies (DSAs) detectable only by flow cytometry (FC) or solid phase assays (SPA) but not CDC is still controversial. We have performed a retrospective analysis of FC cross-matching results in 80 consecutive cadaver kidney allograft recipients. Antibodies against HLA class I and class II antigens were measured by CDC and SPA in sequential samples of sera obtained prior to transplantation. The preoperative cross-match was performed by CDC using magnetically sorted T and B cells from donor spleen. Sera obtained from each patient before and at the time of transplantation were included in the final cross-match. The sample of serum obtained at the time of transplantation was cross-matched retrospectively by FC and analyzed for anti-HLA antibody specificity on high resolution SPA. The actuarial kidney allograft survival at one year was 98%. Two of these eighty patients lost the graft, one due to AMR, the other for reasons unrelated to DSAs. Donor-specific antibodies were detected by FC in 17 of 80 patients, yet only 6 of 17 had an early episode of AMR. This episode was successfully reversed by desensitization therapy using intravenous immunoglobin (IVIG) and plasmapheresis. Flow cytomery cross-matching showed 95% specificity but only 35% sensitivity for prediction of AMR ( p = 0.002). There was a significant correlation between high panel reactive antibodies (PRA) and positive FC cross-matching ( p = 0 .0001), as well as high PRA and AMR ( p = 0.0004 by CDC and 0.0011 by Luminex). Reversible AMR occurred 12–30 days post-transplantation in 8 patients. Of these 8 patients, 3 had no detectable DSAs in spite of C4d positivity, 4 had C4d deposition in conjunction with anti-HLA antibodies, and 1 patient had DSAs (anti-MICA) yet no C4d deposition. We conclude that early initiation of desensitization protocols can prevent transplant failure and that retrospective FC cross-matches may facilitate the diagnosis of AMR. Extensive analysis of patients’ sera using a comprehensive set of tests may contribute to early treatment and better understanding of the mechanism underlying humoral rejection.
doi_str_mv 10.1016/j.humimm.2006.04.012
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For this reason, negative complement-dependent cytotoxicity (CDC) cross-matches between recipient sera and donor T and B lymphocytes have become a mandatory requirement for cadaveric kidney transplantation. However, the significance of donor-specific antibodies (DSAs) detectable only by flow cytometry (FC) or solid phase assays (SPA) but not CDC is still controversial. We have performed a retrospective analysis of FC cross-matching results in 80 consecutive cadaver kidney allograft recipients. Antibodies against HLA class I and class II antigens were measured by CDC and SPA in sequential samples of sera obtained prior to transplantation. The preoperative cross-match was performed by CDC using magnetically sorted T and B cells from donor spleen. Sera obtained from each patient before and at the time of transplantation were included in the final cross-match. The sample of serum obtained at the time of transplantation was cross-matched retrospectively by FC and analyzed for anti-HLA antibody specificity on high resolution SPA. The actuarial kidney allograft survival at one year was 98%. Two of these eighty patients lost the graft, one due to AMR, the other for reasons unrelated to DSAs. Donor-specific antibodies were detected by FC in 17 of 80 patients, yet only 6 of 17 had an early episode of AMR. This episode was successfully reversed by desensitization therapy using intravenous immunoglobin (IVIG) and plasmapheresis. Flow cytomery cross-matching showed 95% specificity but only 35% sensitivity for prediction of AMR ( p = 0.002). There was a significant correlation between high panel reactive antibodies (PRA) and positive FC cross-matching ( p = 0 .0001), as well as high PRA and AMR ( p = 0.0004 by CDC and 0.0011 by Luminex). Reversible AMR occurred 12–30 days post-transplantation in 8 patients. 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For this reason, negative complement-dependent cytotoxicity (CDC) cross-matches between recipient sera and donor T and B lymphocytes have become a mandatory requirement for cadaveric kidney transplantation. However, the significance of donor-specific antibodies (DSAs) detectable only by flow cytometry (FC) or solid phase assays (SPA) but not CDC is still controversial. We have performed a retrospective analysis of FC cross-matching results in 80 consecutive cadaver kidney allograft recipients. Antibodies against HLA class I and class II antigens were measured by CDC and SPA in sequential samples of sera obtained prior to transplantation. The preoperative cross-match was performed by CDC using magnetically sorted T and B cells from donor spleen. Sera obtained from each patient before and at the time of transplantation were included in the final cross-match. 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subjects antibody mediated rejection
antiHLA antibodies
C4d deposition
Cadaver
Female
flow cytometry cross-matches
Graft Rejection - immunology
Humans
Isoantibodies - blood
Kidney Transplantation - immunology
Male
Tissue Donors
Transplantation, Homologous - immunology
title Alloantibodies and the Outcome of Cadaver Kidney Allografts
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