Improved recovery following posttransplant acute renal failure in rat renal isografts with an oral endothelin-A receptor antagonist.

C Braun, S Vetter, T Conzelmann, M Schaub, M Kirchengast, F J van der Woude, P Rohmeiss
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引用次数: 19

Abstract

Background: Delayed renal function after transplantation is a strong predictor of long-term graft survival. As an increased expression of endothelin (ET) has been demonstrated during ischemia/reperfusion injury, we hypothesized that ET-A receptor blockade could improve the recovery of acute renal failure in a rat model of isogeneic kidney transplantation.

Methods: Kidneys of Fisher (F344, RT1(1v1)) rat donors flushed with cooled University of Wisconsin solution were transplanted into bilaterally nephrectomized Fisher rats. Recipient animals were treated orally either with vehicle or the selective ET-A receptor antagonist LU135252 (30 mg/kg/day p.o.) for 14 days. Unilaterally nephrectomized Fisher rats not subjected to ischemia served as controls. No immunosuppression was given. On days 2, 6 and 14, metabolic studies were performed to evaluate endogenous creatinine clearance, fractional sodium excretion, and urinary endothelin excretion. Kidneys were harvested at the end of the experiment for determination of renal ET content and immunohistochemical assessment.

Results: Urinary ET excretion was increased in vehicle-treated isografts compared to uninephrectomized controls after 14 days. Treatment with LU135252 resulted in a significant improvement in creatinine clearance and fractional sodium excretion to the level of uninephrectomized rats after 14 days. Isografts treated with selective ET-A receptor blockade demonstrated a marked reduction in cell surface markers for macrophages/monocytes, T cells, MHC-II, and ICAM-1.

Conclusion: Treatment with the selective ET-A receptor antagonist LU135252 accelerates recovery of renal function after isogeneic renal transplantation and attenuates cellular graft infiltration. This effect could have major implications for the treatment of patients undergoing renal transplantation, as an improved initial renal function may delay the onset of chronic allograft rejection.

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口服内皮素- a受体拮抗剂改善大鼠肾同种移植物移植后急性肾功能衰竭的恢复。
背景:移植后肾功能延迟是移植物长期存活的重要预测指标。由于内皮素(ET)在缺血/再灌注损伤中表达增加,我们假设ET- a受体阻断可以改善大鼠同种异体肾移植模型急性肾功能衰竭的恢复。方法:将Fisher (F344, RT1(1v1))大鼠供体肾脏用冷却的威斯康星大学溶液冲洗后移植到双侧肾切除的Fisher大鼠中。受体动物分别口服载药或选择性ET-A受体拮抗剂LU135252 (30 mg/kg/day, p.o.) 14天。单侧肾切除Fisher大鼠作为对照组。未给予免疫抑制。在第2、6和14天,进行代谢研究以评估内源性肌酐清除率、部分钠排泄和尿内皮素排泄。实验结束时取肾,测定肾ET含量和免疫组化评价。结果:14天后,与未切除肾的对照组相比,经载体处理的同种移植物的尿ET排泄增加。用LU135252治疗14天后,肌酐清除率和部分钠排泄显著改善至未切除肾大鼠的水平。选择性ET-A受体阻断处理的等移植物显示巨噬细胞/单核细胞、T细胞、MHC-II和ICAM-1的细胞表面标记物明显减少。结论:选择性ET-A受体拮抗剂LU135252可加速同种异体肾移植术后肾功能恢复,减轻移植物细胞浸润。这种效应可能对肾移植患者的治疗具有重要意义,因为初始肾功能的改善可能会延迟慢性同种异体移植排斥反应的发生。
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