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霉酚酸酯对长时间冷保存大鼠肾移植的影响。

Effect of mycophenolate mofetil on rat kidney grafts with prolonged cold preservation.

作者信息

Fuller T F, Hoff U, Rose F, Linde Y, Freise C E, Dragun D, Feng S

机构信息

Department of Urology, Charité Universitaetsmedizin Berlin Campus Mitte, Berlin, Germany.

出版信息

Kidney Int. 2006 Aug;70(3):570-7. doi: 10.1038/sj.ki.5001591. Epub 2006 Jun 21.

Abstract

The impact of mycophenolate mofetil (MMF) on initial renal transplant function is not well characterized. We tested how MMF may modulate graft function and survival in a syngeneic rat kidney transplantation model after prolonged cold preservation. Donor kidneys were preserved in University of Wisconsin for either 24 or 39 h prior to transplantation into nephrectomized rats. Recipients received MMF (20 mg/kg/day) or vehicle. Mycophenolic acid (MPA) blood concentrations were measured by high-performance liquid chromatography. The inflammatory response, tubular epithelial proliferation, and histologic damage 3 days post-transplantation were assessed microscopically. In the 24 h cold storage (c.s.) group serum-creatinine was measured. In the 39 h c.s. group 1-week recipient survival was determined. After 24 h of c.s., recipient survival was 100%. The number of T-cell infiltrates was low and not influenced by MMF, whereas renal ED1+ cell infiltration was significantly suppressed by MMF. Tubular cell proliferation was enhanced by MMF. Serum-creatinine levels and renal histology were comparable between MMF and vehicle-treated animals. In the 39 h c.s. group, recipient survival was 20% in MMF-treated vs 90% in vehicle-treated animals (P=0.001). MMF effectively suppressed inflammatory cell infiltration and inhibited tubular cell proliferation. MMF-induced structural damage was most striking in the renal papilla. In rat kidney grafts with moderate preservation injury (24 h c.s.), MMF, given at an immunosuppressive dose, showed predominantly antiinflammatory effects without compromising graft function. In grafts with severe preservation injury (39 h c.s.), MMF caused irreversible structural damage and inhibited tubular cell regeneration resulting in renal failure.

摘要

霉酚酸酯(MMF)对肾移植初期功能的影响尚未得到充分阐明。我们在延长冷保存时间后的同基因大鼠肾移植模型中,测试了MMF如何调节移植肾功能和存活情况。供体肾在威斯康星大学保存24或39小时后,移植入切除肾脏的大鼠体内。受体接受MMF(20mg/kg/天)或赋形剂。采用高效液相色谱法测定霉酚酸(MPA)血药浓度。在移植后3天,通过显微镜评估炎症反应、肾小管上皮细胞增殖和组织学损伤。在24小时冷保存(c.s.)组中,测定血清肌酐。在39小时c.s.组中,确定受体1周存活率。24小时c.s.后,受体存活率为100%。T细胞浸润数量较少,且不受MMF影响,而MMF可显著抑制肾脏ED1+细胞浸润。MMF可增强肾小管细胞增殖。MMF组和赋形剂治疗组动物的血清肌酐水平和肾脏组织学情况相当。在39小时c.s.组中,MMF治疗组受体存活率为20%,而赋形剂治疗组为90%(P=0.001)。MMF可有效抑制炎症细胞浸润并抑制肾小管细胞增殖。MMF诱导的结构损伤在肾乳头最为明显。在具有中度保存损伤(24小时c.s.)的大鼠肾移植中,给予免疫抑制剂量的MMF主要表现出抗炎作用,而不影响移植肾功能。在具有严重保存损伤(39小时c.s.)的移植中,MMF导致不可逆的结构损伤并抑制肾小管细胞再生,从而导致肾衰竭。

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