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BK多瘤病毒相关性肾病期间,移植肾内血树突状细胞抗原-1阳性髓样树突状细胞增加。

Intragraft Blood Dendritic Cell Antigen-1-Positive Myeloid Dendritic Cells Increase during BK Polyomavirus-Associated Nephropathy.

作者信息

Yapici Ünsal, Kers Jesper, Slavujevic-Letic Ivana, Stokman Geurt, Roelofs Joris J T H, van Aalderen Michiel C, Groothoff Jaap W, de Boer Onno J, van der Pant Karlijn A M I, Claessen Nike, Hilbrands Luuk B, Bemelman Frederike J, Ten Berge Ineke J M, Florquin Sandrine

机构信息

Departments of Pathology and.

Departments of Pathology and

出版信息

J Am Soc Nephrol. 2016 Aug;27(8):2502-10. doi: 10.1681/ASN.2015040442. Epub 2015 Dec 23.

Abstract

Although both polyomavirus infection and T cell-mediated rejection (TCMR) are characterized by tubulointerstitial inflammation in the renal allograft, these conditions are treated with opposing therapeutic regimens. To gain more insight into the differences between antiviral and alloimmune responses, we performed a case-control study, in which we immunophenotyped the inflammatory infiltrates in renal biopsy specimens with BK polyomavirus-associated nephropathy (BKPyVAN) and specimens with TCMR. Compared with TCMR, BKPyVAN was diagnosed later after transplantation; therefore, BKPyVAN specimens showed more chronic damage than TCMR specimens showed. However, TCMR and BKPyVAN specimens had comparable levels of tubulointerstitial inflammation. Adjustment for confounders in various multivariable models revealed more blood dendritic cell antigen-1(+) (BDCA-1(+)) myeloid dendritic cells (mDCs) present during BKPyVAN (odds ratio, 2.31; 95% confidence interval, 1.03 to 5.16; P=0.04) than during TCMR. Double immunostaining for SV40 and BDCA-1 showed that, during BKPyVAN, BDCA-1(+) mDCs localized in proximity to the polyomavirus-infected tubular epithelial cells. We ensured that time of biopsy after transplantation was not a confounding factor by including additional specimens with late TCMR and protocol biopsy specimens matched for biopsy time. These additional specimens showed amounts of BDCA-1(+) mDCs comparable with amounts in the early TCMR specimens. These results suggest that BDCA-1(+) mDCs, known to be involved in the antiviral immune response during various viral infections, might have a pivotal role during BKPyVAN infection in the grafted kidney.

摘要

尽管多瘤病毒感染和T细胞介导的排斥反应(TCMR)在肾移植中均以肾小管间质炎症为特征,但这两种情况的治疗方案却截然相反。为了更深入了解抗病毒反应和同种免疫反应之间的差异,我们进行了一项病例对照研究,对肾活检标本中与BK多瘤病毒相关性肾病(BKPyVAN)相关的炎性浸润以及TCMR标本进行了免疫表型分析。与TCMR相比,BKPyVAN在移植后更晚被诊断出来;因此,BKPyVAN标本显示出比TCMR标本更多的慢性损伤。然而,TCMR和BKPyVAN标本的肾小管间质炎症水平相当。在各种多变量模型中对混杂因素进行调整后发现,BKPyVAN期间存在的血液树突状细胞抗原-1(+)(BDCA-1(+))髓样树突状细胞(mDCs)比TCMR期间更多(优势比,2.31;95%置信区间,1.03至5.16;P=0.04)。对SV40和BDCA-1进行双重免疫染色显示,在BKPyVAN期间,BDCA-1(+)mDCs定位于多瘤病毒感染的肾小管上皮细胞附近。我们纳入了晚期TCMR的额外标本以及活检时间匹配的方案活检标本,以确保移植后活检时间不是一个混杂因素。这些额外标本显示BDCA-1(+)mDCs的数量与早期TCMR标本中的数量相当。这些结果表明,已知在各种病毒感染期间参与抗病毒免疫反应的BDCA-1(+)mDCs可能在移植肾BKPyVAN感染期间起关键作用。

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