Dosing Strategies for de Novo Once-daily Extended Release Tacrolimus (LCPT) in Kidney Transplant Recipients
| Status: | Recruiting |
|---|---|
| Conditions: | Renal Impairment / Chronic Kidney Disease |
| Therapuetic Areas: | Nephrology / Urology |
| Healthy: | No |
| Age Range: | 18 - Any |
| Updated: | 11/16/2018 |
| Start Date: | November 12, 2018 |
| End Date: | August 2019 |
| Contact: | Adam Diamond, PharmD |
| Email: | adam.diamond@tuhs.temple.edu |
| Phone: | 215-280-8041 |
Outcomes after kidney transplantation have been significantly enhanced with the advances made
in immunosuppressive therapies. Tacrolimus is currently marketed as an extended-release
once-daily formulation dosing option for patients, decreasing pill burden and possibly
decreasing adverse effects. Some transplant recipients have been shown to have higher dosage
requirements. According to the literature, this can be linked to genetic disparities in the
metabolism of tacrolimus.. This potential complication, where differences on specific genes
alters metabolism of tacrolimus, can increase difficulty in getting to a therapeutic drug
level for immunosuppresants and is one large factor that contributes to the fact that kidney
transplant survival rates differ between patients. Due to the enhanced bioavailability of
Meltdose formulation once-daily extended-release tacrolimus, its de novo use in recent
research and practice has been shown to expedite achievement of target tacrolimus trough
concentrations. De novo use of once-daily tacrolimus formulations is understudied. Through a
prospective investigational study, we aim to determine the optimal strategy for de novo
dosing of once-daily extended release tacrolimus (MeltDose formulation) for kidney transplant
recipients at Temple University Hospital.
in immunosuppressive therapies. Tacrolimus is currently marketed as an extended-release
once-daily formulation dosing option for patients, decreasing pill burden and possibly
decreasing adverse effects. Some transplant recipients have been shown to have higher dosage
requirements. According to the literature, this can be linked to genetic disparities in the
metabolism of tacrolimus.. This potential complication, where differences on specific genes
alters metabolism of tacrolimus, can increase difficulty in getting to a therapeutic drug
level for immunosuppresants and is one large factor that contributes to the fact that kidney
transplant survival rates differ between patients. Due to the enhanced bioavailability of
Meltdose formulation once-daily extended-release tacrolimus, its de novo use in recent
research and practice has been shown to expedite achievement of target tacrolimus trough
concentrations. De novo use of once-daily tacrolimus formulations is understudied. Through a
prospective investigational study, we aim to determine the optimal strategy for de novo
dosing of once-daily extended release tacrolimus (MeltDose formulation) for kidney transplant
recipients at Temple University Hospital.
Patients will be identified when an organ from live or deceased donor becomes available for
kidney transplant. Prior to receiving their kidney transplant, subjects will be screened for
inclusion/exclusion criteria on the day of transplantation. During the pre-operative
preparation for transplant, patients will be consented for surgery and consented for the
study at the same time if they volunteer to be included. The transplant surgeon performing
the transplant operation will be responsible for screening the patients for inclusion and
exclusion criteria as well as obtaining informed consent. Patients will need to provide
informed consent to be included in the study, and will receive a copy of their consent. Each
potential participant will be approached by the transplant surgeon and informed of all
information pertinent to the study prior to providing consent. No advertisements for
recruitment will be performed and no compensation will be provided for participation.
This study is a single center prospective observational study conducted at Temple University
Hospital (TUH). All participants will be consented for all procedures involved in this study.
This study will utilize the QUEST questionnaire (attached) to evaluate the severity of
tremors at 1 month. Data to be collected includes tacrolimus trough levels, study drug
dosing, hemoglobin A1c, incidence and severity of tremors, potassium, glomerular filtration
rate, and rejection episodes.
Day 0 Study drug (tacrolimus) initiated at 0.13/mg/kg/day for all patients (the day of
initiation decided per transplant surgeon discretion)
Day 0-4 Inpatient laboratory parameters checked every 24 hours (serum creatinine, tacrolimus
level, glomerular filtration rate, potassium, blood glucose)
Day 4-30 Outpatient laboratory parameters checked three times weekly on Monday, Wednesday,
and Friday (serum creatinine, tacrolimus level, glomerular filtration rate, potassium, blood
glucose)
Day 30 visit (within 5 days) Draw tacrolimus trough levels, serum creatinine, estimated
glomerular filtration rate, serum potassium, and blood glucose. Complete tremor questionnaire
with participant.
During or prior to Day 30 visit Oral swab performed to be analyzed for testing of metabolic
enzymatic activity (This will be performed to determine ability of the patient to metabolize
tacrolimus)
kidney transplant. Prior to receiving their kidney transplant, subjects will be screened for
inclusion/exclusion criteria on the day of transplantation. During the pre-operative
preparation for transplant, patients will be consented for surgery and consented for the
study at the same time if they volunteer to be included. The transplant surgeon performing
the transplant operation will be responsible for screening the patients for inclusion and
exclusion criteria as well as obtaining informed consent. Patients will need to provide
informed consent to be included in the study, and will receive a copy of their consent. Each
potential participant will be approached by the transplant surgeon and informed of all
information pertinent to the study prior to providing consent. No advertisements for
recruitment will be performed and no compensation will be provided for participation.
This study is a single center prospective observational study conducted at Temple University
Hospital (TUH). All participants will be consented for all procedures involved in this study.
This study will utilize the QUEST questionnaire (attached) to evaluate the severity of
tremors at 1 month. Data to be collected includes tacrolimus trough levels, study drug
dosing, hemoglobin A1c, incidence and severity of tremors, potassium, glomerular filtration
rate, and rejection episodes.
Day 0 Study drug (tacrolimus) initiated at 0.13/mg/kg/day for all patients (the day of
initiation decided per transplant surgeon discretion)
Day 0-4 Inpatient laboratory parameters checked every 24 hours (serum creatinine, tacrolimus
level, glomerular filtration rate, potassium, blood glucose)
Day 4-30 Outpatient laboratory parameters checked three times weekly on Monday, Wednesday,
and Friday (serum creatinine, tacrolimus level, glomerular filtration rate, potassium, blood
glucose)
Day 30 visit (within 5 days) Draw tacrolimus trough levels, serum creatinine, estimated
glomerular filtration rate, serum potassium, and blood glucose. Complete tremor questionnaire
with participant.
During or prior to Day 30 visit Oral swab performed to be analyzed for testing of metabolic
enzymatic activity (This will be performed to determine ability of the patient to metabolize
tacrolimus)
Inclusion Criteria:
Adult patient who is 18 years of age or older receiving a kidney transplant at the Temple
University Hospital's Kidney Transplant Program who are capable of understanding consent
and volunteer to take part in the study
Exclusion Criteria:
Scheduled for multiple organ transplant at enrollment Non-English speaking Pregnant women
Moderate-severe hepatic impairment (Child Pugh > 10 or bilirubin > 2) Existing
contraindications to tacrolimus-based products including known hypersensitivity to
tacrolimus or any other component of the formulation Receiving concomitant medications
known to have strong drug-drug interaction potential with tacrolimus including fluconazole,
voriconazole, posaconazole, isavuconazole, itraconazole, ketoconazole, diltiazem,
verapamil, metronidazole, erythromycin, clarithromycin, rifampin, rifabutin, rifapentine,
phenytoin, fosphenytoin, phenobarbital, primidone, carbamazepine, St. John's Wort,
efavirenz, neivrapine, etravirine, atazanavir, darunavir, fosamprenavir, indinavir,
lopinavir, ritonavir, nelfinavir, saquinavir, tipranavir, cobicistat
We found this trial at
1
site
3401 N Broad St
Philadelphia, Pennsylvania
Philadelphia, Pennsylvania
(215) 707-2000
Phone: 215-280-8041
Temple University Hospital On January 18, 1892 a three-story house at 3403 North Broad Street...
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