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Polyomavirus-associated nephropathy: a comparison of 2 different strategies for immunosuppression reduction.

机译:多瘤病毒相关性肾病:两种不同免疫抑制策略的比较。

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摘要

Polyomavirus-associated nephropathy (PVAN) is an increasing cause of renal allograft dysfunction, but the optimal management of immunosuppression for these patients is unclear. We examined the clinical course of 58 patients with biopsy-proven PVAN diagnosed from 1997 to 2008 at Johns Hopkins Medical Institutions. Immunosuppression management was analyzed as 2 different immunosuppression reduction strategies, the first centered on eliminating a single immunosuppressive drug and reducing the doses of all other immunosuppressive drugs (Strategy A, n = 40), compared with the second, centered on reducing the doses of all immunosuppressive drugs and eliminating none (Strategy B, n = 18). Primary outcome was graft failure, defined as a 50% reduction in estimated glomerular filtration rate, or the need for dialysis within 2 years of PVAN diagnosis. Graft failure developed in 17 (29%) patients during follow-up. In unadjusted and adjusted Cox models, both strategies of immunosuppression reduction had similar efficacy in preventing graft failure (hazard ratio [HR], 0.61; 95% confidence interval, 0.18-2.06; p = 0.43). Rejection after PVAN occurred in 24 of 58 patients and was associated with a 3-fold higher risk of graft failure (HR, 2.99; p = 0.005). Ancillary therapies (cidofovir or leflunomide) were associated with a trend toward faster clearance of viremia (p = 0.65) but were not predictive of outcome.In conclusion, the 2 strategies of immunosuppression reduction had similar efficacy in preventing graft failure. Post-PVAN rejection leads to graft failure. Early repeat allograft biopsy should be considered in the management of PVAN with persistent graft dysfunction.
机译:多瘤病毒相关性肾病(PVAN)是引起同种异体肾功能不全的主要原因,但对于这些患者的免疫抑制的最佳治疗方法尚不清楚。我们检查了约翰霍普金斯大学医学院自1997年至2008年诊断为经活检证实的PVAN的58例患者的临床过程。免疫抑制管理被分析为2种不同的免疫抑制减少策略,第一个以消除单一免疫抑制药物和减少所有其他免疫抑制药物的剂量为中心(策略A,n = 40),而第二个以减少所有免疫抑制剂的剂量为中心免疫抑制药物,且一律不消(策略B,n = 18)。主要结果是移植失败,定义为估计的肾小球滤过率降低50%,或在PVAN诊断后2年内需要透析。在随访期间,有17名(29%)患者发生了移植失败。在未经调整和经调整的Cox模型中,两种降低免疫抑制的策略在预防移植失败方面具有相似的功效(危险比[HR]为0.61; 95%置信区间为0.18-2.06; p = 0.43)。 58例患者中有24例发生PVAN后排斥反应,与移植失败的风险增加3倍相关(HR,2.99; p = 0.005)。辅助疗法(西多福韦或来氟米特)与清除病毒血症的趋势趋于相关(p = 0.65),但不能预示结果。总之,降低免疫抑制的两种策略在预防移植失败方面具有相似的功效。 PVAN后排斥反应会导致移植失败。对于有持续性移植物功能障碍的PVAN,应考虑早期的重复同种异体活检。

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