首页> 外文期刊>American Journal of Transplantation >Reducing Immunosuppression Preserves Allograft Function in Presumptive and Definitive Polyomavirus-Associated Nephropathy
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Reducing Immunosuppression Preserves Allograft Function in Presumptive and Definitive Polyomavirus-Associated Nephropathy

机译:减少免疫抑制可保留同种异体移植功能,在推测性和确定性多瘤病毒相关性肾病中

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Early detection of polyomavirus BK (BKV) viremia and reduction of immunosuppression is recommended for preventing polyomavirus-associated nephropathy (PyVAN), but systematic histological evaluations were not performed in previous studies. We routinely screen for decoy cells and, if positive, measure plasma BKV-loads. In a cohort of 203 consecutive renal transplantations performed from 2005–2008, 38 patients (19%) developed BKV-viremia and were treated with reduction of immunosuppression. Based on subsequent allograft biopsy results and peak BKV-viremia, patients were assigned to three groups: (i) definitive PyVAN (n = 13), (ii) presumptive PyVAN defined by plasma BKV-loads of ≥4 log10 copies/ml (n = 17) and (iii) low BKV-viremia (n = 8). Clearance of BKV-viremia was achieved in 35/38 patients (92%) and subsequent clinical rejection occurred in 3/35 patients (8.6%), both without any difference among the groups. Patients with definitive PyVAN had higher peak plasma BKV-loads and required longer time for clearance (8.8 vs. 4.6 vs. 2.9 months; p = 0.001). However, allograft function remained stable from baseline to last follow-up at 34 months (range 18–60) in all three groups with median serum creatinine of 1.6 mg/dl, 1.6 mg/dl and 1.3 mg/dl, respectively. We conclude that screening for BKV-replication and reduction of immunosuppression is an effective strategy to preserve medium-term allograft function even in patients developing definitive PyVAN.
机译:建议尽早发现多瘤病毒BK(BKV)病毒血症并降低免疫抑制作用,以预防多瘤病毒相关性肾病(PyVAN),但先前的研究未进行系统的组织学评估。我们常规筛查诱饵细胞,如果阳性,则测量血浆BKV负荷。在2005年至2008年进行的203例连续肾脏移植队列中,有38例(19%)患者出现了BKV病毒血症,并接受了免疫抑制治疗。根据随后的同种异体移植活检结果和BKV病毒血症峰值,将患者分为三组:(i)明确的PyVAN(n = 13),(ii)血浆BKV负荷≥4 log 10 < / sub>个/ ml(n = 17)和(iii)低BKV病毒血症(n = 8)。 BKV病毒血症的清除率在35/38例患者中达到了(92%),随后的临床排斥反应在3/35例患者中发生了(8.6%),两组之间没有任何差异。明确的PyVAN患者血浆BKV峰值负荷较高,需要更长的清除时间(8.8 vs. 4.6 vs. 2.9个月; p = 0.001)。然而,所有三个组的同种异体移植物功能从基线到最后一次随访在34个月(范围18-60)均保持稳定,血清肌酐中位数分别为1.6 mg / dl,1.6 mg / dl和1.3 mg / dl。我们得出的结论是,即使在正在发展确定性PyVAN的患者中,筛查BKV复制和减少免疫抑制也是保留中期同种异体移植功能的有效策略。

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