Unbound Plasma, Total Plasma, and Whole-Blood Tacrolimus Pharmacokinetics Early After Thoracic Organ Transplantation

Sikma, Maaike A.; Maarseveen, Erik M. van; Hunault, Claudine C.; Moreno, J. Marta; Graaf, E.A. van de; Kirkels, J. H.; Verhaar, Marianne C.; Grutters, Jan C.; Kesecioğlu, Jozef; Lange, Dylan W. de; Huitema, Alwin D. R.

doi:10.1007/s40262-019-00854-1

Cited by 28 publications

(48 citation statements)

References 32 publications

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“…There appeared to be a stronger direct correlation between dose and C Graft than between dose and C 0Blood . An important source of variability in the relationship between dose and C 0Blood is likely to be the significant binding of tacrolimus to red blood cells and plasma proteins 40 . Since only unbound tacrolimus is available to be taken up (either passively or actively) from plasma into the allograft kidney, the stronger correlation may be due to C Graft better reflecting unbound plasma tacrolimus concentrations and hence dose.…”

Section: Discussionmentioning

confidence: 99%

Tacrolimus dose, blood concentrations and acute nephrotoxicity, but not CYP3A5/ABCB1 genetics, are associated with allograft tacrolimus concentrations in renal transplant recipients

Sallustio

Noll

et al. 2021

Brit J Clinical Pharma

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Aims Long‐term use of the immunosuppressant tacrolimus is limited by nephrotoxicity. Following renal transplantation, the risk of nephrotoxicity may be determined more by allograft than by blood tacrolimus concentrations, and thus may be affected by donor CYP3A5 and ABCB1 genetics. Little is known regarding factors that determine tacrolimus intrarenal exposure. Methods This study investigated the relationship between trough blood (C0Blood) and allograft (CGraft) tacrolimus concentrations and tacrolimus dose, haematocrit, genetics, acute nephrotoxicity, rejection status, delayed graft function, and time post‐transplant. C0Blood and CGraft were quantified in 132 renal transplant recipients together with recipient and donor CYP3A5 (rs776746) and ABCB1 3435 (rs1045642) genotypes. Results C0Blood ranged from 2.6 to 52.3 ng/mL and CGraft from 33 to 828 pg/mg tissue. Adjusting for dose, recipients who were CYP3A5 expressors had lower C0Blood compared to nonexpressors, whilst delayed graft function was associated with higher C0Blood. Linear regression showed that the significant predictors of CGraft were C0Blood (point‐wise P = 7 × 10−10), dose (P = .004) acute nephrotoxicity (P = .002) and an interaction between C0Blood and acute tacrolimus nephrotoxicity (P = .0002), with an adjusted r2 = 0.35 and no contribution from donor or recipient CYP3A5 or ABCB1 genotype. The association between CGraft and acute nephrotoxicity depended on one very high CGraft (828 pg/mg tissue). Conclusions Recipient and donor CYP3A5 and ABCB1 3435C>T genotypes are not determinants of allograft tacrolimus exposure in kidney transplant recipients. However, tacrolimus dose and C0Blood were significant predictors of CGraft, and the relationship between C0Blood and CGraft appeared to differ in the presence or absence of acute nephrotoxicity.

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Section: Discussionmentioning

confidence: 99%

Tacrolimus dose, blood concentrations and acute nephrotoxicity, but not CYP3A5/ABCB1 genetics, are associated with allograft tacrolimus concentrations in renal transplant recipients

Sallustio

Noll

et al. 2021

Brit J Clinical Pharma

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“…For tacrolimus, which displays similar erythrocyte partitioning as everolimus, various authors have advocated for the implementation of TDM based on haematocrit-normalised whole-blood concentrations across different fields of transplantation [39][40][41][42][43]. Additionally, a recent consensus paper on tacrolimus TDM included recommendations for further investigation of alternative TDM strategies, including haematocrit normalisation, to explain and resolve the highly variable tacrolimus efficacy in patient subpopulations [37].…”

Section: Discussionmentioning

confidence: 99%

Model-Informed Precision Dosing of Everolimus: External Validation in Adult Renal Transplant Recipients

et al. 2020

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Background and Objective The immunosuppressant everolimus is increasingly applied in renal transplantation. Its extensive pharmacokinetic variability necessitates therapeutic drug monitoring, typically based on whole-blood trough concentrations (C 0). Unfortunately, therapeutic drug monitoring target attainment rates are often unsatisfactory and patients with on-target exposure may still develop organ rejection. As everolimus displays erythrocyte partitioning, haematocrit-normalised wholeblood exposure has been suggested as a more informative therapeutic drug monitoring marker. Furthermore, model-informed precision dosing has introduced options for more sophisticated dose adaptation. We have previously developed a mechanistic population pharmacokinetic model, which described everolimus plasma pharmacokinetics and enabled estimation of haematocrit-normalised whole-blood exposure. Here, we externally evaluated this model for its utility for model-informed precision dosing. Methods The retrospective dataset included 4123 pharmacokinetic observations from routine clinical therapeutic drug monitoring in 173 renal transplant recipients. Model appropriateness was confirmed with a visual predictive check. A fit-forpurpose analysis was conducted to evaluate whether the model accurately and precisely predicted a future C 0 or area under the concentration-time curve (AUC) from prior pharmacokinetic observations. Bias and imprecision were expressed as the mean percentage prediction error (MPPE) and mean absolute percentage prediction error (MAPE), stratified on 6 months post-transplant. Additionally, we compared dose adaptation recommendations of conventional C 0-based therapeutic drug monitoring and C 0-or AUC-based model-informed precision dosing, and assessed the percentage of differences between observed and haematocrit-normalised C 0 (∆C 0) and AUC (∆AUC) exceeding ± 20%. Results The model showed adequate accuracy and precision for C 0 and AUC prediction at ≤ 6 months (

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“…Les données en transplantation thoracique (cardiaque, pulmonaire et cardio-pulmonaire) sont anciennes et les recommandations datant de 20 ans font état d'une cible de 15 à 20 ng/mL qui n'est plus d'actualité [12]. Deux études récentes, l'une en transplantation cardiaque et l'autre en transplantation pulmonaire, suggèrent que des concentrations résiduelles au-delà de 15 ng/mL au cours des 2 premières semaines post-transplantation sont péjoratives au plan rénal pour les patients [13,14]. Les données disponibles à ce jour ne permettent pas de recommander une minimisation plus importante de l'exposition au tacrolimus dans ces indications.…”

Section: En Transplantation Rénaleunclassified

Synthèse des recommandations de l’International Association of Therapeutic Drug Monitoring and Clinical Toxicology (IATDMCT) sur le suivi thérapeutique pharmacologique du tacrolimus

et al. 2020

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Synthèse des recommandations de l'International Association of Therapeutic Drug Monitoring and Clinical Toxicology (IATDMCT) sur le suivi thérapeutique pharmacologique du tacrolimus* Summary of the recommendations of the International Association of Therapeutic Drug Monitoring and Clinical Toxicology (IATDMCT) on the therapeutic drug monitoring of tacrolimusRecommandations IATDMCT sur le STP du tacrolimus

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Unbound Plasma, Total Plasma, and Whole-Blood Tacrolimus Pharmacokinetics Early After Thoracic Organ Transplantation

Cited by 28 publications

References 32 publications

Tacrolimus dose, blood concentrations and acute nephrotoxicity, but not CYP3A5/ABCB1 genetics, are associated with allograft tacrolimus concentrations in renal transplant recipients

Tacrolimus dose, blood concentrations and acute nephrotoxicity, but not CYP3A5/ABCB1 genetics, are associated with allograft tacrolimus concentrations in renal transplant recipients

Model-Informed Precision Dosing of Everolimus: External Validation in Adult Renal Transplant Recipients

Synthèse des recommandations de l’International Association of Therapeutic Drug Monitoring and Clinical Toxicology (IATDMCT) sur le suivi thérapeutique pharmacologique du tacrolimus

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