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Conversion of liver allograft recipients from cyclosporine to FK506 immunosuppressive therapy— a clinicopathologic study of 96 patients

机译:肝同种异体移植受者从环孢素转换为FK506免疫抑制疗法-96例患者的临床病理研究

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摘要

The effect of conversion from cyclosporine-steroid immunosuppression to the new agent FK506 was studied in 96 liver allograft recipients who were experiencing graft dysfunction or cyclosporine toxicity. Patients were stratified according to the cause of graft dysfunction that ultimately led to conversion to FK506. Response to FK506 introduction was monitored pathologically and biochemically. The outcome of a switch from CsA to FK506 was highly favorable in patients experiencing acute and the early stages of chronic rejection, despite optimal conventional therapy. Patients with later stages of chronic rejection did not respond to conversion to FK506 and most eventually lost their liver grafts in this process. Patients in whom we had difficulty separating chronic rejection from chronic persistent or low-grade chronic active hepatitis were mostly unaffected by conversion to FK506. Active hepatitis was a poor indication for conversion, because most of the patients experienced graft failure or died from liver failure. As a group, there was no statistically significant change in renal function 180 days after conversion to FK506. These findings expand the experience with FK506 in human liver allograft recipients. © 1992 by Williams and Wilkins.
机译:在96名经历移植物功能障碍或环孢素毒性的肝脏同种异体移植受者中,研究了从环孢素-类固醇免疫抑制转换为新药FK506的效果。根据移植功能障碍的原因对患者进行分层,最终导致其转化为FK506。病理和生化监测对FK506引入的反应。尽管有最佳的常规治疗方法,但对于经历急性和早期慢性排斥反应的患者,从CsA转换为FK506的结果还是非常有利的。患有慢性排斥反应后期的患者对FK506的转化无反应,大多数患者最终在此过程中失去了肝脏移植物。我们难以将慢性排斥反应与慢性持续性或低度慢性活动性肝炎区分开的患者大多不受改用FK506的影响。活动性肝炎是转化的不良指征,因为大多数患者经历了移植物衰竭或死于肝衰竭。整体而言,转换为FK506后180天肾脏功能没有统计学上的显着变化。这些发现扩展了FK506在人类肝脏同种异体移植受者中的经验。 ©1992,威廉姆斯和威尔金斯。

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