Pharmacokinetics of Sirolimus and Tacrolimus in Liver Transplant Recipients With Tacrolimus Toxicity

Phase 3TerminatedNCT01709136

University of Pittsburgh3 enrolled

Overview

Pharmacokinetics of Tacrolimus and Sirolimus alone and in combination in liver transplant recipients.

Liver transplant patients receiving tacrolimus, and who experience side effects such as hypertension and renal dysfunction, will be converted to sirolimus with low-dose tacrolimus, or Tacrolimus withdrawal. This study will evaluate allograft function by serial clinical lab testing, the pharmacokinetics of sirolimus and tacrolimus, the glomerular filtration rate (GFR) and the potential side effect of sirolimus, such as marrow suppression and hyperlipidemia. Two pharmacokinetic evaluations are planned: once around the third post-transplant month and another one at about 12 months. Expected outcomes are, a better understanding of sirolimus pharmacokinetic parameters over time in pediatric/adult liver recipients and early efficacy and safety data of the sirolimus as a non-nephrotoxic alternative to tacrolimus.

Study Type

INTERVENTIONAL

Allocation

Purpose

TREATMENT

Masking

NONE

Enrollment

Conditions

Hypertension

Interventions

SirolimusDRUG

Single dose SRL pharmacokinetics and TAC steady state pharmacokinetics: This phase is applicable to both sets of patients: those with nephrotoxicity and those with hypertension. Patients will receive a single dose of SRL of 2 mg/m2. Blood sampling will be performed over a 24 hour stay in the Children's Hospital of Pittsburgh's Pediatric Clinical and Translational Research Center (PCTRC) - See more at: http://www.chp.edu/research/our-facilities/pctrc, and the sampling for 48 hour and 72 hour PK studies can be done at the outpatient lab. This phase can either be performed immediately after the 12-hour iothalamate GFR evaluation, or a few days later at the convenience of the subject.

Eligibility

Sex: ALLMin age: 1 YearMax age: 18 Years

Medical Language ↔ Plain English

Inclusion Criteria: * Recipients of primary liver (cadaver/liver, whole/segmental) transplants 5- 30 years old. * Rejection-free post-transplant course for at least 3 months * Renal dysfunction (15% decrease in age-adjusted calculated creatinine clearance) * Hypertension requiring anti-hypertensive mediations. * Informed consent. * Weight ≥15 kg. Exclusion Criteria: * Rejection or infections within 3 months of enrollment. * Intent to continue TAC * Active participation in ongoing studies of immunosuppressive agents. * Lack of informed consent. * Pregnant or breast feeding * HIV positive

Outcomes

Primary Outcomes

Early and Late Pharmacokinetics of Sirolimus (SRL)

To evaluate early and late pharmacokinetics of Sirolimus (SRL) , and safety and efficacy of conversion from tacrolimus (TAC) to sirolimus in liver transplant recipients who have been stable for at least 3 months, and who have early nephrotoxicity and/or hypertension due to use of tacrolimus.

Time frame: 1 year

Secondary Outcomes

PK Parameters for Tacrolimus and Sirolimus

pharmacokinetics (PK) of SRL after a single dose and after steady state has been achieved; and the pharmacokinetics of tacrolimus once at steady state

Time frame: 12 months

SRL Can Substitute TAC

Whether Sirolimus can substitute Tacrolimus in the stable post-transplant state, without compromising allograft function

Time frame: 12 months

SRL Prevent TAC-related Side Effects

Whether SRL can prevent or minimize progression of selected TAC-related side-effects such as renal dysfunction as measured by clearance of iothalamate (Glomerular filtration rate \< 80 mL/min/1.73 m2) and hypertension (blood pressure \> 140/90 mm Hg)

Time frame: 1 year

Data from ClinicalTrials.gov

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