Thrombotic microangiopathy in a renal allograft : single-center Five-year experience
Thrombotic microangiopathy (TMA) is devastating for renal transplantation (RT) causing graft/ patient loss. We present 5-year experience of TMA in RT in retrospective study of indicated renal allograft biopsies with TMA. Patient–donor demographics and associated histological findings with respect to...
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Veröffentlicht in: | Saudi journal of kidney diseases and transplantation 2020-11, Vol.31 (6), p.1331-1343 |
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Zusammenfassung: | Thrombotic microangiopathy (TMA) is devastating for renal transplantation (RT)
causing graft/ patient loss. We present 5-year experience of TMA in RT in retrospective study of
indicated renal allograft biopsies with TMA. Patient–donor demographics and associated
histological findings with respect to transplants under tolerance induction protocol (Group 1)
were compared with patients transplanted under triple immunosuppression (Group 2). Statistical
analysis was performed using IBM SPSS Statistics version 20. Sixty-one (4.1%) of 1520 biopsies
[Group 1:17 (1.9%)/882, Group 2:44 (6.9%)/638] revealed TMA. Tacrolimus trough levels were
normal. There was no evidence of systemic involvement in any patient. Mean age was 36.8 years
with 70.6% males, HLA-match, 2.6/6, and the most common original disease unknown (41.2%)
in Group 1, and 35.9 years with 86.4% males, HLA-match, 2.1/6, and the most common original
disease unknown (50%) in Group 2. Biopsies were performed at mean 5.1-year posttransplant in
Group 1 and 2.3 years in Group 2. Acute TMA constituted 47% Group 1 and 43.2% Group 2
biopsies; of these, antibody-mediated rejections were observed in 58.8%, T-cell mediated
rejections in 11.8%, tacrolimus toxicity in 76.5%, and other findings in 35.3% Group 1; and 61.4%, 25%, 50%, and 18.2%, respectively, in Group
2 biopsies. Higher rejection activity scores
were more in Group 2. Postbiopsy 1- and 5- year patient survival was 94.1%, 86.9% in
Group 1 and 92.1%, 88.3% in Group 2; 1- and
4-year graft survival was 52.9%, 15.9% in
Group 1 and 20.3%, 5.4% in Group 2. TMA
was poor prognosticator for RT, especially
under triple immunosuppression. Antibody- mediated rejection and tacrolimus toxicity
were more prone to TMA. |
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ISSN: | 1319-2442 2320-3838 |
DOI: | 10.4103/1319-2442.308342 |