Clinical determinants of calcineurin inhibitor disposition: a mechanistic review

Vanhove, Thomas; Annaert, Pieter

doi:10.3109/03602532.2016.1151037

Cited by 131 publications

(180 citation statements)

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“…105 Expressers of the CYP3A5 enzyme (as is more often the case in black and Asian patients) do require higher dosages to reach therapeutic tacrolimus exposure. [105][106][107] The recently developed prolonged-release formulation in tablet form (also known as LCP-tacrolimus) is released and absorbed more distally in the gut. 105,106 This newer formulation of prolonged-release tacrolimus in tablets has shown some differences in terms of pharmacokinetics but longterm clinical outcome data is yet to be established.…”

Section: Strategies For Managing Nonadherencementioning

confidence: 99%

“…[105][106][107] The recently developed prolonged-release formulation in tablet form (also known as LCP-tacrolimus) is released and absorbed more distally in the gut. 105,106 This newer formulation of prolonged-release tacrolimus in tablets has shown some differences in terms of pharmacokinetics but longterm clinical outcome data is yet to be established. 106 After absorption, tacrolimus diffuses extensively in blood cells and tissues.…”

Section: Strategies For Managing Nonadherencementioning

confidence: 99%

“…There is extensive presystemic metabolism by the CYP3A enzymes in the gut wall and first-pass metabolism in liver, which limits its oral bioavailability. 105 Expressers of the CYP3A5 enzyme (as is more often the case in black and Asian patients) do require higher dosages to reach therapeutic tacrolimus exposure. [105][106][107] The recently developed prolonged-release formulation in tablet form (also known as LCP-tacrolimus) is released and absorbed more distally in the gut.…”

Section: Strategies For Managing Nonadherencementioning

confidence: 99%

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Practical Recommendations for Long-term Management of Modifiable Risks in Kidney and Liver Transplant Recipients

et al. 2017

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Short-term patient and graft outcomes continue to improve after kidney and liver transplantation, with 1-year survival rates over 80%; however, improving longer-term outcomes remains a challenge. Improving the function of grafts and health of recipients would not only enhance quality and length of life, but would also reduce the need for retransplantation, and thus increase the number of organs available for transplant. The clinical transplant community needs to identify and manage those patient modifiable factors, to decrease the risk of graft failure, and improve longer-term outcomes. COMMIT was formed in 2015 and is composed of 20 leading kidney and liver transplant specialists from 9 countries across Europe. The group's remit is to provide expert guidance for the long-term management of kidney and liver transplant patients, with the aim of improving outcomes by minimizing modifiable risks associated with poor graft and patient survival posttransplant. The objective of this supplement is to provide specific, practical recommendations, through the discussion of current evidence and best practice, for the management of modifiable risks in those kidney and liver transplant patients who have survived the first postoperative year. In addition, the provision of a checklist increases the clinical utility and accessibility of these recommendations, by offering a systematic and efficient way to implement screening and monitoring of modifiable risks in the clinical setting. 12 Department of Gastroenterology and Hepatology, Erasmus MC, University Hospital Rotterdam, the Netherlands. 13 Department of Gastroenterology and Hepatology, University Hospitals KU Leuven, Belgium.14 Abdominal Transplant Surgery, Microbiology and Immunology Department, University Hospitals KU Leuven, Belgium. 15 Department of Hepatology and Liver Transplantation, Reina Sofía University Hospital, IMIBIC, CIBERehd, Spain. www.transplantjournal.com S1 S olid organ transplantation has evolved from an experimental procedure to an established treatment option for many types of end-stage organ failure. Both patient and graft outcomes are continuing to improve, and 1-year patient and graft survival currently exceed 80%.1,2 However, survival rates gradually decline over the long term. In kidney transplant, 5-and 10-year graft survival rates in Europe are 77% and 56%, and for liver transplant, 64% and 54% (Figures 1 and 2). 3,4 Although most European countries have seen an increase in both living and deceased donation, transplantation is not available to all who would benefit from the procedure, and there is considerable morbidity and mortality for those listed for transplant.6 Therefore, maximizing long-term graft survival and reducing the need for retransplantation is paramount, not only in improving outcomes for the recipients but also for those awaiting a graft. The improvement in outcomes is predominantly due to reduction in (Transplantation. 2017;101:S1-S41). The authors were approached by Astellas to discuss the practical implementation o...

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Section: Strategies For Managing Nonadherencementioning

confidence: 99%

Section: Strategies For Managing Nonadherencementioning

confidence: 99%

Section: Strategies For Managing Nonadherencementioning

confidence: 99%

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Practical Recommendations for Long-term Management of Modifiable Risks in Kidney and Liver Transplant Recipients

et al. 2017

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“…8,9 Pharmacokinetics After oral administration, tacrolimus undergoes extensive first-pass effects via p-glycoprotein and intestinal and hepatic cytochrome P450 3A (CYP3A) enzymes. 10 Tacrolimus is primarily eliminated from the body in the bile by hepatic metabolism, and less than 1% of unchanged drug is excreted in the urine. 11 The oral bioavailability of tacrolimus is low and exhibits large intra-and interindividual variability, ranging from 4% to 89% (mean around 25% in liver and RT recipients and in patients with renal impairment).…”

Section: Mechanisms Of Actionmentioning

confidence: 99%

Untitled

Shrestha

2017

Exp Clin Transplant

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Tacrolimus, a calcineurin inhibitor, has been the cornerstone of immunosuppressive regimens in renal transplant over 2 decades. This has significantly improved the outcomes of renal transplant, including reduction of acute rejection episodes, improvement of renal function and graft survival, and reduction of some of the adverse effects associated with cy closporine. However, use of tacrolimus is associated with a number of undesirable effects, such as nephrotoxicity, posttransplant diabetes mellitus, neurotoxicity, and cosmetic and electrolyte disturbances. To alleviate these effects, several strategies have been adopted to minimize or eliminate tacrolimus from maintenance regimens of immuno suppression, with some success. This review focuses on advancements in the under standing of the basic science related to tacrolimus and the clinical evidences that have examined the efficacy and safety of tacrolimus in renal transplant over the past 2 decades and highlights the future directions.

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“…The authors presume that the identified sets of gene variants (because of their distribution with oxidoreductase/monooxygenase activity) are causally linked to tacrolimus metabolism and thus exposure. It is important to note, however, that in the first 3 mo after transplantation, a number of clinical factors known to affect tacrolimus bioavailability closely covary with tacrolimus dosing and influence dose-corrected exposure, for example, graft function or dysfunction, gastrointestinal motility, hematocrit, albumin, corticosteroid tapering, and concomitant drugs (drug-drug interactions) (2). The fact that these factors were not corrected for increases the risk of overfitting the PLS1 models by modeling variability that is likely to be determined by clinical factors.…”

Section: To the Editormentioning

confidence: 99%

Predictive Modeling of Tacrolimus Dose Requirements: “All That Is Gold Does Not Glitter”

Vanhove

2017

American Journal of Transplantation

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We read, with interest, the paper by Damon et al on predictive models based on selected gene variants that explain variability in tacrolimus dose-corrected trough levels (C 0 ) in renal recipients (1). We want to share some of our critiques regarding methodology and interpretation of data.First, we suggest not using the term "predictive modeling" in a setting of multiple gene variant sets that variably associate with concurrent tacrolimus C 0 at different time points after transplantation. Validation of predictive models would require accurate estimation of tacrolimus dose requirements in independent populations either at similar, separate time points (PLS1 models) or for all time points (PLS2 models; e.g. in the "Necker cohort," although this was not performed). The authors presume that the identified sets of gene variants (because of their distribution with oxidoreductase/monooxygenase activity) are causally linked to tacrolimus metabolism and thus exposure. It is important to note, however, that in the first 3 mo after transplantation, a number of clinical factors known to affect tacrolimus bioavailability closely covary with tacrolimus dosing and influence dose-corrected exposure, for example, graft function or dysfunction, gastrointestinal motility, hematocrit, albumin, corticosteroid tapering, and concomitant drugs (drug-drug interactions) (2). The fact that these factors were not corrected for increases the risk of overfitting the PLS1 models by modeling variability that is likely to be determined by clinical factors. Why would the majority of gene variants that were relevant on day 60 no longer be so on day 90? With the exception of previously identified genetic variants of enzymes involved in tacrolimus metabolism (figure 2 in Damon et al; singlenucleotide polymorphisms [SNPs] are shown in dark red/orange for the PSL1 model, and underlined CYP3A5 and CYP3A4 SNPs contributed to the PLS2 model), the sets of SNPs that are linked at only one or two time points with tacrolimus exposure are purely associative (78 of 85 SNPs) and are not explanatory, let alone predictive, unless validated. The collapse of complexity in the PSL2 models and the concurrent drop in performance (R² = 0.28) illustrate this point quite clearly.Second, the rationale for separate analyses in the fixed-dose subgroup and the CYP3A5 nonexpressers in the adapted dose group is not clear. The majority of white patients (80% CYP3A5*3/*3) are initially overexposed with a standard tacrolimus loading dose (0.2 mg/ kg) (3-5). Because all tacrolimus concentrations (whether in the fixed-or adapted-dose group) are considered to be in steady state on day 10 (no dose changes allowed until then), the differences in PSL1 model performance in these subgroups (supplementary table 3 in Damon et al) cannot be explained by different dosing strategies, as the authors suggest (1). For later time points (after day 10), this could theoretically be the case because more dose adaptations were performed in the fixed-dose subgroup, resulting in more "non-steady-sta...

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Clinical determinants of calcineurin inhibitor disposition: a mechanistic review

Cited by 131 publications

References 301 publications

Practical Recommendations for Long-term Management of Modifiable Risks in Kidney and Liver Transplant Recipients

Practical Recommendations for Long-term Management of Modifiable Risks in Kidney and Liver Transplant Recipients

Untitled

Predictive Modeling of Tacrolimus Dose Requirements: “All That Is Gold Does Not Glitter”

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