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肾移植活检组织中MHC I类相关链B(MICB)分子的表达

Expression of MHC class I-related Chain B (MICB) molecules on renal transplant biopsies.

作者信息

Quiroga Isabel, Salio Mariolina, Koo Dicken D H, Cerundolo Lucy, Shepherd Dawn, Cerundolo Vincenzo, Fuggle Susan V

机构信息

Nuffield Department of Surgery, University of Oxford, John Radcliffe Hospital, Oxford, United Kingdom.

出版信息

Transplantation. 2006 Apr 27;81(8):1196-203. doi: 10.1097/01.tp.0000205788.05322.42.

Abstract

BACKGROUND

MICA and MICB (MHC class I-related chain A and B) are polymorphic genes that encode molecules related to MHC class I and are expressed on epithelial cells in response to stress. Incompatible donor MIC antigens can stimulate antibody production in transplant recipients. This study was designed to determine MICB expression in kidney pretransplant and any subsequent changes in expression following transplantation and to correlate changes with inflammatory markers and clinical events.

METHODS

Paired renal biopsies obtained from living donor (n=10) and cadaveric allografts (n=50) before and 7 days posttransplant were stained for MICB, leukocytic infiltration, and HLA class II antigens.

RESULTS

Variable tubular MICB expression was evident in donor biopsies [high 6/60 (10%), low/negative 13/60 (22%), intermediate 41/60 (68%)]. Following transplantation, MICB was up-regulated on renal tubules of 17/60 (28%) biopsies and was associated with MHC class II antigen induction (P=0.02) and leukocyte infiltration (P=0.01). Acute tubular necrosis leading to delayed graft function (DGF) and acute rejection (AR) cause cellular stress within the transplanted kidney. We found a strong association between up-regulation of MICB and cellular stress, 15/17 biopsies with up-regulated MICB expression had AR and/or DGF (P=0.003).

CONCLUSIONS

This is the first study demonstrating variable levels of MICB expression in kidneys before transplantation and induction of MICB expression following renal transplantation. MICB expression is associated with HLA class II antigen induction, leukocytic infiltration of the graft and cellular stress in the transplanted kidney. Expression of MICB could contribute significantly to the alloimmune response in mismatched donors and recipients.

摘要

背景

MICA和MICB(主要组织相容性复合体I类相关链A和B)是多态性基因,编码与主要组织相容性复合体I类相关的分子,并在应激反应时在上皮细胞中表达。不相容的供体MIC抗原可刺激移植受者产生抗体。本研究旨在确定肾移植前MICB的表达情况以及移植后表达的任何后续变化,并将这些变化与炎症标志物和临床事件相关联。

方法

对活体供肾(n = 10)和尸体同种异体肾移植(n = 50)在移植前及移植后7天获取的配对肾活检组织进行MICB、白细胞浸润和HLA II类抗原染色。

结果

供体活检组织中可见不同程度的肾小管MICB表达[高表达6/60(10%),低表达/阴性13/60(22%),中等表达41/60(68%)]。移植后,60份活检组织中有17份(28%)肾小管的MICB表达上调,且与MHC II类抗原诱导(P = 0.02)和白细胞浸润(P = 0.01)相关。导致移植肾功能延迟恢复(DGF)和急性排斥反应(AR)的急性肾小管坏死会在移植肾内引起细胞应激。我们发现MICB上调与细胞应激之间存在强烈关联,17份MICB表达上调的活检组织中有15份发生了AR和/或DGF(P = 0.003)。

结论

这是第一项证明肾移植前肾脏中MICB表达水平各异以及肾移植后MICB表达被诱导的研究。MICB表达与HLA II类抗原诱导、移植肾的白细胞浸润以及移植肾内的细胞应激相关。MICB的表达可能在不匹配的供体和受体的同种免疫反应中起重要作用。

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