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改良型环孢素制剂之间的生物等效性是否意味着疗效相同?

Does bioequivalence between modified cyclosporine formulations translate into equal outcomes?

作者信息

Taber David J, Baillie G Mark, Ashcraft Elizabeth E, Rogers Jeffrey, Lin Angello, Afzal Fuad, Baliga Prabhakar, Rajagopalan P R, Chavin Kenneth D

机构信息

School of Pharmacy, Wingate University, Wingate, NC, USA.

出版信息

Transplantation. 2005 Dec 15;80(11):1633-5. doi: 10.1097/01.tp.0000188688.15639.03.

Abstract

Neoral was replaced with a generic cyclosporine formulation on our hospital formulary. We compared outcomes for de novo kidney transplant recipients who either received Gengraf (n=88) or Neoral (n=100) in a single-center, retrospective review. As compared to patients who received Neoral, patients who received Gengraf were significantly more likely to have an acute rejection episode (39% vs. 25%, P=0.04), more likely to have a second rejection episode (13% vs. 4%; P=0.03), or to have received an antibody preparation to treat acute rejection (19% vs. 8%; P=0.02). Patients treated with Gengraf had a higher degree of intrapatient variability for cyclosporine trough concentrations as determined by %CV (P<0.05). The incidence of acute rejection at 6 months posttransplant was significantly higher in patients who received Gengraf compared to Neoral. A larger, prospective analysis is warranted to compare these formulations of cyclosporine in de novo kidney transplant recipients.

摘要

我院药品处方集上的新山地明已被环孢素普通制剂取代。我们在一项单中心回顾性研究中,比较了初发肾移植受者接受金格福(n = 88)或新山地明(n = 100)后的结局。与接受新山地明的患者相比,接受金格福的患者发生急性排斥反应的可能性显著更高(39% 对 25%,P = 0.04),发生第二次排斥反应的可能性更高(13% 对 4%;P = 0.03),或接受抗体制剂治疗急性排斥反应的可能性更高(19% 对 8%;P = 0.02)。通过变异系数(%CV)测定,接受金格福治疗的患者环孢素谷浓度的患者内变异性程度更高(P < 0.05)。与新山地明相比,接受金格福的患者移植后6个月时急性排斥反应的发生率显著更高。有必要进行一项更大规模的前瞻性分析,以比较初发肾移植受者中这些环孢素制剂。

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