Acute Cellular Rejection with CD20‐Positive Lymphoid Clusters in Kidney Transplant Patients Following Lymphocyte Depletion
Lymphoid clusters (LC) containing CD20‐positive B cells in kidney allografts undergoing acute cellular rejection (ACR) have been identified in small studies as a prognostic factor for glucocorticoid resistance and graft loss. Allograft biopsies obtained during the first episode of ACR in 120 recipie...
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Veröffentlicht in: | American journal of transplantation 2007-04, Vol.7 (4), p.949-954 |
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Zusammenfassung: | Lymphoid clusters (LC) containing CD20‐positive B cells in kidney allografts undergoing acute cellular rejection (ACR) have been identified in small studies as a prognostic factor for glucocorticoid resistance and graft loss. Allograft biopsies obtained during the first episode of ACR in 120 recipients were evaluated for LC, immunostained with CD20 antibody, and correlated with conventional histopathologic criteria, response to treatment and outcome. LC were found in 71 (59%) of the 120 biopsies. All contained CD20 positive B cells that accounted for 5–90% of the LC leukocyte content. The incidence of LC was highest in the patients who had no lymphoid depletion or had been treated with Thymoglobulin preconditioning (79% vs. 75%, respectively) compared to 37% in patients pretreated with Campath (p = 0.0001). Banff 1a/1b ACR were more frequent in the LC‐positive than the LC‐negative group (96% vs. 80%, respectively; p = 0.0051). With a posttransplant follow‐up of 953 ± 430 days, no significant differences were detected between LC‐postitive and LC‐negative groups in time to ACR, steroid resistance, serum creatinine and graft loss. CD20+LC did not portend glucocorticoid resistance or worse short to medium term outcomes. CD20+LC may represent a heterogenous collection in which there may be a small still to be fully defined unfavorable subgroup.
Our results indicate that renal allograft biopsies of acute rejection with lymphoid clusters containing variable proportions of B‐cells stained by CD20 mAb represent a heterogeneous collection rather than a distinct clinicopathologic entity. |
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ISSN: | 1600-6135 1600-6143 |
DOI: | 10.1111/j.1600-6143.2007.01737.x |