De-novo use of generic tacrolimus (Adoport) in renal transplant recipients: A single center experience from Türkiye

N. Koç, T. Yıldırım, Ş. Yılmaz, Yunus Erdem
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Abstract

Objective: Renal transplantation is the best treatment for end-stage kidney disease, and tacrolimus has become an important immunosuppressive treatment for kidney transplant patients since it was introduced. After the first generic tacrolimus has been approved by the FDA, studies have begun to compare the effectiveness and safety of generic tacrolimus with the original tacrolimus. When using generic immunosuppressive therapies, it is also necessary to ensure that it provides adequate immunosuppression and does not cause severe toxicity. This study aims to compare clinical outcomes, including acute rejection, graft loss and adverse reactions, in patients receiving brand tacrolimus (Prograf, Astellas Pharma, U.S.) or generic tacrolimus (Adoport, Sandoz, UK) from the start of kidney transplant therapy. Study Design: Renal transplant recipients between 1 January 2015-1 March 2020 were screened retrospectively. All patients receiving de novo generic tacrolimus (n:51) and randomly selected 102 control renal transplant recipients receiving original tacrolimus were included in this study. Materials and Methods: We evaluated and recorded demographic, clinical and laboratory data including age, gender, primary kidney disease, donor type (live or dead), induction and death regimen, tacrolimus dose, tacrolimus through levels, serum creatinine, biopsy-confirmed acute rejection episodes, delayed transplant function, positive BK polyomavirus in the urine, BK polyomavirus-related nephropathy, cytomegalovirus infection in 1-year follow-up. Results: Most of the patients were male (64.1%) with a mean age of 38.3 years. There was no significant difference in demographic characteristics between the original and generic tacrolimus groups. No differences were found in terms of creatinine levels, total daily dose of tacrolimus and tacrolimus trough levels at discharge and the first year. Additionally, biopsy-confirmed acute rejection in the following year after transplantation, BKPyV positivity in urine, BKPyVAN, CMV viremia and adverse reactions related to tacrolimus were similar between the two groups. Conclusion: With this study, we aimed to contribute to the literature with our experience on the use of generic tacrolimus from our country. As a result of our study, we noted that generic tacrolimus can be safely preferred for de-novo use with close drug-level monitoring because it is an immunosuppressant agent with a narrow therapeutic index. There is a continuing need for randomized prospective-designed and multi-centric studies with a wide range of patients.
肾移植受者重新使用通用他克莫司(Adoport):土耳其单个中心的经验
目的:肾移植是治疗终末期肾病的最佳方法,他克莫司自问世以来已成为肾移植患者的重要免疫抑制剂。美国食品及药物管理局(FDA)批准首款他克莫司仿制药后,开始有研究将他克莫司仿制药与原版他克莫司的有效性和安全性进行比较。本研究旨在比较肾移植治疗开始后接受品牌他克莫司(Prograf,Astellas Pharma,美国)或普通他克莫司(Adoport,Sandoz,英国)患者的临床结果,包括急性排斥反应、移植物丢失和不良反应:研究设计:对 2015 年 1 月 1 日至 2020 年 3 月 1 日期间的肾移植受者进行回顾性筛选。研究设计:回顾性筛选 2015 年 1 月 1 日至 2020 年 3 月 1 日期间的肾移植受者,纳入所有接受全新通用他克莫司治疗的患者(n:51)和随机抽取的 102 名接受原研他克莫司治疗的对照组肾移植受者:我们评估并记录了人口统计学、临床和实验室数据,包括年龄、性别、原发性肾脏疾病、供体类型(活体或死体)、诱导和死亡方案、他克莫司剂量、他克莫司通过水平、血清肌酐、活检证实的急性排斥反应发作、移植功能延迟、尿液中BK多瘤病毒阳性、BK多瘤病毒相关肾病、巨细胞病毒感染:大多数患者为男性(64.1%),平均年龄为 38.3 岁。原研他克莫司组和普通他克莫司组的人口统计学特征无明显差异。在肌酐水平、他克莫司每日总剂量以及出院时和第一年的他克莫司谷值水平方面,也未发现差异。此外,两组患者在移植后第二年经活检证实的急性排斥反应、尿液中BKPyV阳性、BKPyVAN、CMV病毒血症以及与他克莫司相关的不良反应均相似:通过这项研究,我们旨在为文献提供我国使用通用他克莫司的经验。研究结果表明,非专利他克莫司是一种治疗指数较窄的免疫抑制剂,因此可以在密切监测药物浓度的情况下安全地优先用于新药治疗。目前仍需要对广泛的患者进行随机前瞻性设计和多中心研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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