The effect of tacrolimus conversion from immediate- to extended-release formulation on renal function in renal transplant patients: a meta-analysis

Chao, Sheng; Jia, Lei; Zhu, Kejing; Chen, Luobei; Niu, Yulin

doi:10.3389/fphar.2023.1226647

Cited by 2 publications

(1 citation statement)

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“…The use of prolonged- or extended-release formulations of tacrolimus, usually taken once a day, is a part of the clinical standard of care for kidney transplant recipients ( 1 ). Recently, a meta-analysis indicated that the conversion from IR-Tac twice daily to ER-Tac once daily may decrease serum creatinine in kidney transplant recipients with a follow-up duration of more than 48 weeks, but at the same time, eGFR remained unchanged ( 11 ). At least many randomized controlled studies could show that the administration of ER-Tac once daily with less peak levels (and therefore in total reduced maximum plasma concentrations) does not appear to have an impact on either the efficacy or safety of this formulation and is an effective immunosuppressant treatment in kidney transplant recipients ( 7 , 8 , 12 , 13 ).…”

Section: Discussionmentioning

confidence: 99%

The use of extended-release tacrolimus twice a day might be beneficial for selected kidney transplant recipients: a case report

Füessl,

Kreuzer,

Nierychlewski

et al. 2024

Front. Med.

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The calcineurin inhibitor tacrolimus, which is available as an immediate- or extended-release formulation, is the standard-of-care immunosuppression after kidney transplantation with low rejection rates, especially in the first year after transplantation. However, its highly variable metabolism rate, narrow therapeutic window, and nephrotoxic side effects require close drug monitoring and individual dosing. Here, we describe first the application of extended-release tacrolimus (ER-Tac) twice daily with beneficial effects in a kidney transplant recipient under extensive therapeutic drug monitoring. A 47-year-old female kidney transplant recipient, who was identified as a fast metabolizer for tacrolimus, presented with declining allograft function and low tacrolimus through levels over time and 8 years after a second kidney transplantation despite the administration of high doses of ER-Tac once daily. Therefore, the area under the concentration–time curve (AUC) showed exceedingly high blood levels of ER-Tac. The latest biopsy of the kidney transplant showed arteriolar hyalinosis with pole vessel stenosis as a sign of chronic transplant vasculopathy and transplant glomerulopathy as a sign of chronic humoral rejection. After the exclusion of other options for immunosuppressive therapy due to the patient’s high immunological risk, the patient was switched from ER-Tac once daily to ER-Tac twice daily. After switching to ER-Tac twice daily, the AUC for oral tacrolimus decreased and the transplant function improved despite higher tacrolimus trough levels and a lower total dose administered. This case highlights the importance of careful therapeutic drug monitoring with the performance of an AUC in the follow-up management of kidney transplant recipients.

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