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J Nephropathol. 2017;6(4): 290-303.
doi: 10.15171/jnp.2017.48

Scopus ID: 85036577410
  Abstract View: 4972
  PDF Download: 2439

Original Article

Long-term outcomes after ABO-incompatible kidney transplantation; a single-center French study

Zhiyar Abdulrahman 1, Hamza Bennani Naciri 1, Asma Allal 1, Federico Sallusto 2, Bénédicte Debiol 3, Laure Esposito 1, Céline Guilbeau-Frugier 4,5, Nassim Kamar 1,6,5, Lionel Rostaing 1,6,5*

1 Department of Nephrology and Organ Transplantation, CHU Rangueil, TSA 50032 Toulouse, France
2 Department of Urology, Andrology, and Transplantation, CHU Rangueil, TSA 50032 Toulouse, France
3 Etablissement Français du Sang de Midi-Pyrénées, CHU Purpan, Toulouse, France
4 Histopathology Department, Oncopole, Toulouse, France
5 Université Paul Sabatier, Toulouse, France
6 INSERM U563, IFR–BMT, CHU Purpan, Toulouse, France
*Corresponding Author: *Corresponding author: Professor Lionel Rostaing, Department of Nephrology and Organ Transplantation, CHU Rangueil, TSA 50032 Toulouse, France. , Email: LRostaing@chu-grenoble.fr

Abstract

Background: ABO-incompatible (ABOi) is as efficient as ABO-compatible (ABOc) kidneytransplantation in the setting of live-donation.

Objectives: To evaluate the long-term outcomes (i.e. >6 months) of 44 consecutive ABOi living-donor kidney-transplants (KTx). The results were compared to those from 44 ABOc KTx that were matched with ABOi-patients on age, gender, and date of transplantation.

Patients and Methods: With regards to immunosuppression (IS) only ABOi-patients received pre-transplant IS, that included rituximab. Induction therapy relied significantly more frequently on basiliximab in ABOc- than in ABOi-patients 77.2% vs. 38.6% (P = 0.0002). Post-transplant IS relied only on tacrolimus/mycophenolic acid and steroids in ABOipatients, whereas some ABOc-patients were alternatively on cyclosporine (13.6%)/everolimus (11.3%) and no steroids (7%), respectively (P = 0.05).

Results: In ABOi-patients there was no isoagglutinin titer rebound posttransplant. At last follow-up patient and graft survival was similar in the two groups, as well as kidneyallograft function. Acute rejection rates (cellular, humoral, or mixed) were similar across both groups (ABOi: 22.7%; ABOc: 20.4%). With regards to bacterial and viral infections the only significant difference between the two groups was that at month three there were
significantly more BKV viruria in ABOi (25%) vs. 6.8% in ABOc (P = 0.03). De novo donor-specific alloantibody were detected in 13.6% ABOi and 4.5% ABOc patients (ns). Readmission rates in our department for less than two days were more frequent for ABOi conversely readmission rates for more than two days was similar across the groups.

Conclusions: ABOi-kidney transplantation after desensitization provides in the long-term same results as those observed in live-donor ABOc-kidney transplantation.


Implication for health policy/practice/research/medical education:

We are facing more and more end-stage renal disease (ESRD) patients; of these a large proportion are waitlisted for a kidney transplant. However, due to the scarcity of deceased donors we have to develop live-kidney donor programs. In the setting of living-donation we can face with either ABO and/or HLA incompatible transplantation. ABO incompatible kidney transplantation is associated as we demonstrated in this study with very good long-term results, i.e. similar to those obtained with ABO compatible kidney transplantation provided desensitization is implemented at pre-transplant.

Please cite this paper as: Abdulrahman Z, Bennani Naciri H, Allal A, Sallusto F, Debiol B, Esposito L. Long-term outcomes after ABO-incompatible kidney transplantation; a single-center French study. J Nephropathol. 2017;6(4):290-303. DOI: 10.15171/jnp.2017.48.

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Submitted: 28 Oct 2016
Accepted: 20 Mar 2017
ePublished: 07 Apr 2017
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