Features of acute rejection that increase risk for chronic rejection.

Humar A; Kerr S; Gillingham KJ; Matas AJ

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Features of acute rejection that increase risk for chronic rejection.

机译：急性排斥反应的特征增加了慢性排斥反应的风险。

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BACKGROUND: Acute rejection (AR) has been shown to be a significant risk factor for chronic rejection (CR) in kidney transplant recipients, yet many recipients with AR do not progress to CR. The purpose of this study was to determine if certain AR episodes are associated with a worse prognosis. METHODS: The study group consisted of 279 kidney transplant recipients, all treated for a single episode of biopsy-proven AR. All AR episodes were initially treated with steroids; steroid-resistant rejection was managed with an antibody preparation. RESULTS: First, by univariate techniques, we determined the clinical impact of severity of AR (as estimated by delta creatinine [dCr], defined as the change in baseline serum creatinine level 6 weeks after AR treatment) on two different endpoints--biopsy-proven CR and graft survival. Irrespective of 6-week dCr, all recipients with AR had a significantly increased risk of CR vs. those with no AR (P<0.01). Recipients with dCr between 0.5 and 1.0 mg/dl had a significantly higher incidence of CR vs. those with dCr <0.5 mg/dl (P<0.05), but a significantly lower incidence vs. those with dCr >1.0 mg/dl (P<0.05). We then performed multivariate analysis. We used severity of AR in addition to other variables (e.g., timing of AR, donor age) to determine which factors were most associated with risk for CR and graft loss. Risk for CR increased with AR episodes occurring >6 months after transplant (relative risk [RR] = 3.8, P = 0.005); with moderate or severe (vs. mild) AR episodes (RR = 2.7, P = 0.05); and with dCr >0.5 mg(dl (vs. <0.5 mg/dl) at 6 weeks after AR treatment (RR = 2.3, P = 0.1). Findings were similar when graft survival (death-censored) was the endpoint instead of CR. CONCLUSIONS: All AR episodes are associated with some increase in the risk for CR. But AR episodes occurring >6 months after transplant and those of increased severity (as assessed qualitatively by histologic grading and quantitatively by dCr) confer the greatest risk. Recipients with these risk factors could be targeted with measures to decrease their risk for CR, including trials of novel immunosuppressive regimens.

机译：背景：急性排斥反应（AR）已被证明是肾移植接受者慢性排斥反应（CR）的重要危险因素，但是许多AR接受者并未发展为CR。这项研究的目的是确定某些AR发作是否与预后不良有关。方法：研究组由279名肾移植受者组成，均接受了单次活检证实的AR治疗。所有AR发作最初都使用类固醇治疗。类固醇抗性排斥反应通过抗体制剂来控制。结果：首先，通过单变量技术，我们确定了AR严重程度对两种不同研究终点的临床影响（活检的结果由δ肌酐[dCr]估计，定义为AR治疗后6周血清肌酐水平的变化）。证实的CR和移植物存活率。与6周的dCr无关，所有AR接受者的CR风险均显着高于非AR接受者（P <0.01）。 dCr介于0.5和1.0 mg / dl之间的接受者的CR发生率明显高于dCr <0.5 mg / dl（P <0.05）的接受者，但与dCr> 1.0 mg / dl的接受者的CR发生率明显降低（P <0.05）。然后，我们进行了多元分析。除了其他变量（例如AR的时间，供体的年龄）外，我们还使用了AR的严重性来确定哪些因素与CR和移植物丢失的风险最相关。移植后6个月内发生AR发作，CR风险增加（相对风险[RR] = 3.8，P = 0.005）;中度或重度（相对轻度）AR发作（RR = 2.7，P = 0.05）;在AR治疗后6周时dCr> 0.5 mg（dl（vs. <0.5 mg / dl））（RR = 2.3，P = 0.1）。当以移植物存活率（死亡检查）代替CR作为终点时，发现相似结论：所有AR发作均与CR风险的增加有关，但AR发作发生在移植后6个月以上，而严重程度升高（通过组织学分级定性评估，并通过dCr定量评估）的AR发作风险最大。这些危险因素可以通过降低CR风险的措施来针对，包括新型免疫抑制方案的试验。

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《Transplantation: Official Journal of the Transplantation Society 》 |1999年第8期| 共4页
作者
Humar A; Kerr S; Gillingham KJ; Matas AJ;
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正文语种 eng
中图分类外科手术学 ;
关键词
Graft Rejection; Kidney Transplantation; Protein Isoforms; Creatinine; 移植物排斥; 肾移植;

机译：Graft Rejection;Kidney Transplantation;Protein Isoforms;Creatinine;移植物排斥;肾移植;

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1. Features of acute rejection that increase risk for chronic rejection. [J] . Humar A, Kerr S, Gillingham KJ, Transplantation: Official Journal of the Transplantation Society . 1999 ,第8期

机译：急性排斥反应的特征增加了慢性排斥反应的风险。
2. Incidence, timing, and risk factors for acute and chronic rejection. [J] . Neuberger J Liver transplantation and surgery: official publication of the American Association for the Study of Liver Diseases and the International Liver Transplantation Society . 1999 ,第4Suppla1期

机译：急性和慢性排斥反应的发生率，时间和危险因素。
3. Proton pump inhibitors do not increase the risk of acute rejection. [J] . G A J van Boekel, C H H Kerkhofs, F van de Logt, The Netherlands journal of medicine. . 2014 ,第2期

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5. Raman spectroscopic modeling of T-lymphocyte activation and detection of acute renal allograft rejection. [D] . Brown, Kristian L. 2010

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6. The grafted fetal rat pancreas: features of development and rejection. [O] . P. R. Millard, J. F. Garvey, E. L. Jeffery, 1980

机译：移植的胎鼠胰腺：发育和排斥的特征。
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Features of acute rejection that increase risk for chronic rejection.

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