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早期急性排斥反应在大鼠肾再移植模型中对慢性排斥反应的作用。

Contribution of early acute rejection episodes to chronic rejection in a rat kidney retransplantation model.

作者信息

Tullius S G, Nieminen M, Bechstein W O, Jonas S, Steinmüller T, Qun Y, Pratschke J, Graser E, Sinha P, Volk H D, Neuhaus P, Tilney N L

机构信息

Department of Surgery, Medical Immunology and Clinical Chemistry, University Hospital Charité-Virchow, Berlin, Germany.

出版信息

Kidney Int. 1998 Feb;53(2):465-72. doi: 10.1046/j.1523-1755.1998.00757.x.

Abstract

Chronic graft rejection represents the single most important risk factor for unsatisfactory long-term results after organ transplantation. In addition to various alloantigen dependent and independent factors, acute rejection episodes have been cited as a major immunological risk factor. However, the effects of acute rejection episodes on long-term graft outcome remains unknown. To examine the influence of a single early rejection event on ultimate graft outcome, acutely rejecting rat kidney grafts were retransplanted sequentially into syngeneic rats and their functional and structural behavior assessed over time. LEWxBNF1 kidney allografts and LEW isografts were removed from their LEW recipients after three, four, five and seven days (N = 12/group/time period) and retransplanted into donor strain hosts. The grafts were followed functionally and harvested four, eight, and 32 weeks later. Urinary protein excretion was measured weekly. Kidneys were examined morphologically and immunohistologically using monoclonal antibodies (mAbs) against macrophages (ED-1), T cells and their subsets (CD5, CD4, CD8), MHC class II expression (OX3) and adhesion molecules (ICAM-1 and LFA-1alpha). The mean standard time +/- SD of non-retransplanted allografts was 14.5 +/- two days; isografts functioned indefinitely. At five and seven days, acutely rejecting allografts showed massive cellular infiltrates associated with extensive necrosis. These changes could not be reversed by retransplantation and the syngeneic recipients later died of renal failure. In contrast, most allografts retransplanted earlier in the process recovered completely when retransplanted after three (12 of 12 allografts) and four (7 of 12 allografts) days. During the subsequent follow-up period, urinary protein excretion was comparable in retransplanted allografts and isografts. The increased mononuclear cell infiltration in non-retransplanted allografts seen at three and four days was only occasionally observed during the follow-up period after retransplantation. Only a few sclerosed glomeruli (approximately 15%), mild arterial changes and minimal cellular infiltrates were observed by 32 weeks, which were similar to that seen in retransplanted isografts. A single acute rejection episode was completely reversible and did not progress to chronic rejection if retransplanted into syngeneic donors when the inflammatory changes are still early. Those results demonstrate the critical effect of alloantigen-dependent events on chronic graft deterioration, and indicate that prompt and aggressive treatment of initial acute rejection episodes are beneficial to protect against late deleterious changes in the graft.

摘要

慢性移植排斥是器官移植后长期效果不理想的最重要单一风险因素。除了各种依赖和不依赖同种异体抗原的因素外,急性排斥反应已被视为主要的免疫风险因素。然而,急性排斥反应对移植长期结果的影响尚不清楚。为了研究单次早期排斥事件对最终移植结果的影响,将急性排斥的大鼠肾移植依次重新移植到同基因大鼠体内,并随时间评估其功能和结构变化。在3、4、5和7天后(每组/时间段N = 12)从LEW受体中取出LEWxBNF1同种异体肾移植和LEW同基因移植,然后重新移植到供体品系宿主中。对移植肾进行功能跟踪,并在4、8和32周后采集样本。每周测量尿蛋白排泄量。使用抗巨噬细胞(ED-1)、T细胞及其亚群(CD5、CD4、CD8)、MHC II类表达(OX3)和粘附分子(ICAM-1和LFA-1α)的单克隆抗体(mAb)对肾脏进行形态学和免疫组织学检查。未重新移植的同种异体肾移植的平均标准存活时间±标准差为14.5±2天;同基因移植可无限期发挥功能。在第5天和第7天,急性排斥的同种异体肾移植出现大量细胞浸润并伴有广泛坏死。这些变化不能通过重新移植逆转,同基因受体随后死于肾衰竭。相比之下,在该过程中早期重新移植的大多数同种异体肾移植在3天(12个同种异体肾移植中的12个)和4天(12个同种异体肾移植中的7个)后重新移植时完全恢复。在随后的随访期内,重新移植的同种异体肾移植和同基因移植的尿蛋白排泄量相当。在重新移植后的随访期内,仅偶尔观察到在3天和4天时未重新移植的同种异体肾移植中单核细胞浸润增加。到32周时,仅观察到少数硬化肾小球(约15%)、轻度动脉改变和极少的细胞浸润,这与重新移植的同基因移植所见相似。如果在炎症变化仍处于早期时将单次急性排斥的移植肾重新移植到同基因供体中,其完全可逆且不会进展为慢性排斥。这些结果证明了同种异体抗原依赖性事件对慢性移植恶化的关键作用,并表明对初始急性排斥反应进行及时、积极的治疗有利于预防移植后期的有害变化。

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