Transplantation Direct (Apr 2024)

Modifying Tacrolimus-related Toxicity After Liver Transplantation Comparing Life Cycle Pharma Tacrolimus Versus Extended-released Tacrolimus: A Multicenter, Randomized Controlled Trial

  • Midas B. Mulder, PharmD,
  • Bart van Hoek, MD, PhD,
  • Wojtek G. Polak, MD, PhD,
  • Ian P.J. Alwayn, MD, PhD,
  • Brenda C.M. de Winter, PharmD, PhD,
  • Sarwa Darwish Murad, MD, PhD,
  • Elke Verhey-Hart, BSc,
  • Lara Elshove, MSc,
  • Nicole S. Erler, Dipl-Stat, PhD,
  • Dennis A. Hesselink, MD, PhD,
  • Caroline M. den Hoed, MD, PhD,
  • Herold J. Metselaar, MD, PhD

DOI
https://doi.org/10.1097/TXD.0000000000001612
Journal volume & issue
Vol. 10, no. 4
p. e1612

Abstract

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Background. The aim of this open-label, multicenter, randomized controlled study was to investigate whether the life cycle pharma (LCP)-tacrolimus compared with the extended-release (ER)-tacrolimus formulation results in a difference in the prevalence of posttransplant diabetes, hypertension and chronic kidney disease (CKD) at 12 mo after liver transplantation. Methods. Patients were 1:1 randomized to either of the 2 tacrolimus formulations. The primary endpoint was defined as a composite endpoint of any of 3 events: sustained (>3 mo postrandomization) posttransplant diabetes, new-onset hypertension, and/or CKD, defined as estimated glomerular filtration rate 3 m during the follow-up. Results. In total, 105 patients were included. In the intention-to-treat analysis, a statistically significant lower proportion of liver transplant recipients in the LCP-tacrolimus group reached the composite primary endpoint at 12 mo compared with the ER-tacrolimus group (50.9% [27/53], 95% confidence interval [CI], 37.9%-63.9% versus 71.2% [37/52], 95% CI, 57.7%-81.7%; risk difference: 0.202; 95% CI, 0.002-0.382; P = 0.046). No significant difference was found in the per protocol analysis. In the intention-to-treat and per protocol population, fewer liver transplant recipients in the LCP-tacrolimus group developed CKD and new-onset hypertension compared with the ER-tacrolimus group. No differences in rejection rate, graft and patient survival were found. Conclusions. A statistically significant and clinically relevant reduction in the prevalence of the composite primary endpoint was found in the LCP-tacrolimus group compared with the ER-tacrolimus group in the first year after liver transplantation with comparable efficacy.