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经皮肾移植活检中浆细胞浸润的临床及病理意义

The clinical and pathologic implications of plasmacytic infiltrates in percutaneous renal allograft biopsies.

作者信息

Meehan S M, Domer P, Josephson M, Donoghue M, Sadhu A, Ho L T, Aronson A J, Thistlethwaite J R, Haas M

机构信息

Department of Pathology, University of Chicago, Chicago, IL 60637, USA.

出版信息

Hum Pathol. 2001 Feb;32(2):205-15. doi: 10.1053/hupa.2001.21574.

Abstract

Plasmacytic infiltrates in renal allograft biopsies are uncommon and morphologically distinctive lesions that may represent variants of acute rejection. This study sought significant clinical and pathologic determinants that might have influenced development of these lesions and assessed their prognostic significance. Renal allograft biopsies (n = 19), from 19 patients, with tubulointerstitial inflammatory infiltrates containing abundant plasma cells, composing 32 +/- 8% of the infiltrating mononuclear cells, were classified using Banff '97 criteria. Clonality of the infiltrates was determined by immunoperoxidase staining for kappa and lambda light chains and polymerase chain reaction for immunoglobulin heavy-chain gene rearrangements, using V(H) gene framework 3 and JH consensus primers. In situ hybridization for Epstein-Barr virus encoded RNA (EBER) was performed in 17 cases. The clinical features, histology, and outcome of these cases were compared with kidney allograft biopsies (n = 17) matched for time posttransplantation and type of rejection by Banff '97 criteria, with few plasma cells (7 +/- 5%). Sixteen of 19 biopsies (84%) with plasmacytic infiltrates had EBER-negative (in 14 cases tested) polyclonal plasma cell infiltrates that were classifiable as acute rejection (types 1A [4], 1B [10], and 2A [2]). These biopsies were obtained between 10 and 112 months posttransplantation. Graft loss from acute and/or chronic rejection was 50% at 1 year and 63% at 3 years, and the median time to graft failure was 4.5 months after biopsy. There was no significant difference in overall survival or time to graft failure compared with the controls. Three of 19 biopsies (16%) had EBER-negative polyclonal plasmacytic hyperplasia, mixed monoclonal and polyclonal polymorphous B cell hyperplasia, and monoclonal plasmacytoma-like posttransplantation lymphoproliferative disease (PTLD) and were obtained at 17 months, 12 weeks, and 7 years after transplantation, respectively. Graft nephrectomies were performed at 1, 19, and 5 months after biopsy, respectively. Plasmacytic infiltrates in renal allografts comprise a spectrum of lesions from acute rejection to PTLD, with a generally poor prognosis for long-term graft survival.

摘要

肾移植活检中的浆细胞浸润是罕见的且形态独特的病变,可能代表急性排斥反应的变异型。本研究探寻了可能影响这些病变发生发展的重要临床和病理决定因素,并评估了它们的预后意义。对19例患者的肾移植活检标本(n = 19)进行分类,这些标本的肾小管间质炎性浸润中含有丰富的浆细胞,占浸润单核细胞的32±8%,采用Banff '97标准进行分类。通过免疫过氧化物酶法检测κ和λ轻链以及使用V(H)基因框架3和JH共有引物进行免疫球蛋白重链基因重排的聚合酶链反应来确定浸润细胞的克隆性。17例病例进行了爱泼斯坦 - 巴尔病毒编码RNA(EBER)的原位杂交。将这些病例的临床特征、组织学和转归与17例肾移植活检标本进行比较,这些对照标本在移植后时间和Banff '97标准的排斥反应类型上相匹配,浆细胞较少(7±5%)。19例有浆细胞浸润的活检标本中有16例(84%)EBER阴性(14例检测),多克隆浆细胞浸润可分类为急性排斥反应(1A类[4例]、1B类[10例]和2A类[2例])。这些活检标本在移植后10至112个月获得。1年时因急性和/或慢性排斥反应导致的移植肾丢失率为50%,3年时为63%,活检后移植肾失功的中位时间为4.5个月。与对照组相比,总体生存率或移植肾失功时间无显著差异。19例活检标本中有3例(16%)分别在移植后17个月、12周和7年出现EBER阴性的多克隆浆细胞增生、混合性单克隆和多克隆多形性B细胞增生以及单克隆浆细胞瘤样移植后淋巴增殖性疾病(PTLD)。分别在活检后1个月、19个月和5个月进行了移植肾切除。肾移植中的浆细胞浸润包括从急性排斥反应到PTLD的一系列病变,对移植肾长期存活的预后通常较差。

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