Tacrolimus Associated Tremors in Liver Transplantation: Immediate-Release Versus Extended-Release Formulations (LCP-TAC)

University of British Columbia

Status and phase

Enrolling

Phase 4

Conditions

Tremor

Liver Transplantation

Tacrolimus

Neurotoxicity

Immunosuppression

Treatments

Drug: Tacrolimus, Immediate Release, Oral

Drug: Tacrolimus Extended Release Oral Tablet

Study type

Interventional

Funder types

Other

Identifiers

NCT05089604

H20-01688

Details and patient eligibility

About

This is a randomized open label study in de novo liver transplant recipients that aims to compare the risk of tacrolimus induced tremors with once daily extended-release formulation, Envarsus, versus the twice daily immediate-release formulation. Both formulations of tacrolimus are currently approved for the prevention of rejection in liver transplant patients.

Full description

Purpose: This study is designed to evaluate the incidence and severity of tremors with two different tacrolimus formulations (LCPT versus IR-TAC) when administered in combination with mycophenolate and short term corticosteroids in de novo liver transplant (LT) recipients.

Hypothesis: In de novo liver transplant recipients, an LCPT-based immunosuppression regimen, in combination with mycophenolate and short term steroids offers improved neurotoxicity profile as evidenced by lower incidence and severity of tremors and treatment discontinuation when compared to an identical regimen using twice-daily immediate-release tacrolimus.

Rationale: Tacrolimus is the first line immunosuppressive agent in all organ transplantation and its use is associated with improved patient and graft outcomes. Neurotoxicity including headaches and tremors are amongst common dose limiting toxicities associated with tacrolimus early after liver transplantation. Mitigation strategies include dosage reduction or switch to CSA, both of which can put patient at risk of rejection and other toxicities. LCPT is a new extended release formulation with improved PK parameters and evidence of improved tolerability (lower risk of tremors) in renal transplant population. In this study, we will compare the incidence and severity of tremors associated with IR-TAC, which is currently standard of care at our institution, with LCPT, which is a new dosage form added to the hospital formulary. We will be using wearable sensors to assess the severity of tremors. Furthermore, the objective and systematic documentation of tremor severity during the first 8 weeks after transplantation will provide granular data that will elucidate the natural history of tacrolimus induced tremors early post liver transplantation.

Research design: This is a single centre, prospective, randomized, open label, parallel group trial in adult de novo liver transplant recipients. Patients will be randomized (1:1) to either LCPT or IR-TAC, both groups will receive mycophenolate and short term steroids according to the standard of care protocol. This is a superiority study.

Enrollment

124 estimated patients

Sex

All

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Adults aged 18 years or older
Recipients of a first-time liver transplant
eGFR more than 30 ml/min on the day of tacrolimus initiation
All patients who are eligible to initiate Tacrolimus within 7 days post-liver transplant
Informed consent

Exclusion criteria

Recipients of prior organ transplant
Need for hemodialysis either prior or following liver transplantation
Recipients of living donor liver or split deceased donor liver allografts
Recipients of combined liver/kidney transplants
Recipients receiving liver allografts from donors with HCV viremia (detected through nucleic acid testing or other means)
Patients with a history of tremor prior to transplantation including essential tremors, Parkinson's or Parkinsonian syndromes
Patients receiving concomitant medications known to induce tremors such as dopamine blocking agents
Baseline TSH, T3, T4 indicating hyperthyroidism