Rationale: The combination of azathioprine and prednisone is the first-line treatment for autoimmune hepatitis (AIH), a chronic inflammatory disease of the liver. Complete biochemical remission (CR) is the first treatment goal in autoimmune hepatitis. CR is determined by AST and ALT and IgG within the reference range. CR is not reached in a substantial proportion of AIH patients: after one year 50%, after three years around 20% did not achieve CR. Without CR ongoing hepatitis leads to progression towards fibrosis and eventually (decompensated) cirrhosis. Not achieving CR is the most important risk factor for the need for liver transplantation or liver related death, independent of age and presence of cirrhosis. Tacrolimus (TAC) and mycophenolate mofetil (MMF) are frequently used to prevent rejection in kidney and liver transplant patients. In AIH patients with insufficient response or intolerance to first-line therapy in retrospective cohort studies with MMF 0-57% and with TAC 20-95% CR was reached. Objective: The aim of this study is to compare the effectiveness of TAC with MMF as a second line treatment for AIH. Proportion of patients with CR after 12 months of treatment will be the primary outcome parameter to determine effectivity. Study design: Randomized open-label two arm study. Patients will be randomized between treatment with TAC or MMF. Study population: Patients with AIH with an incomplete response (no CR) to first-line treatment are eligible for this study. Intervention: In the TAC group baseline treatment will be replaced by tacrolimus. In the MMF group baseline treatment will be replaced by MMF. The current dose of prednisolone, or at least 5 mg daily, will be continued in both arms. After achieving CR prednisolone will be tapered according to protocol. Main study parameters/endpoints: Difference in proportion of patients with CR at 12 months (normalization of ALT, AST and IgG) between the TAC and MMF treatment group. Secondary parameters: * Safety and tolerability of TAC and MMF treatments * Difference in proportion of patients with CR at 6 months (normalization of ALT, AST and IgG) between the TAC and MMF treatment group. * Difference in ALT, AST and IgG at 6 and 12 months versus baseline * Difference in fibrogenesis and fibrosis parameters between groups and before and after treatment * Difference in quality of life between groups and before and after treatment
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
86
Mycophenolate mofetil will be started at a dose 500mg twice daily. When tolerated and an AUC within range, patients will be titrated to 1000mg twice daily at week two.
Meltdose tacrolimus will be started at a dose of 0.07 mg/kg/day. The drug will be taken orally once-daily in the morning. Dose will be adjusted to reach target AUC and trough levels.
Jeroen Bosch Ziekenhuis
's-Hertogenbosch, Netherlands
NOT_YET_RECRUITINGReinier de Graaf Gasthuis
Delft, Netherlands
NOT_YET_RECRUITINGMedisch Spectrum Twente
Enschede, Netherlands
NOT_YET_RECRUITINGLeiden University Medical Center
Leiden, Netherlands
RECRUITINGMaastricht University Medical Center +
Maastricht, Netherlands
NOT_YET_RECRUITINGUniversity Medical Center Utrecht
Utrecht, Netherlands
NOT_YET_RECRUITINGComplete biochemical remission
The proportion of patients with CR after 12 months of treatment with TAC compared to MMF in patients with AIH with an incomplete response to first-line treatment.
Time frame: 52 weeks
Safety and Tolerability
Number and severity of side effects; Rate of stopping treatment due to side effects; serum creatinin \& potassium; Blood pressure; Blood glucose levels and incidence of new onset diabetes; Number of (opportunistic) infections; tremor; diarrhea
Time frame: 52 weeks
Proportion of patients with complete biochemical remission after 6 months
Defined as ALT, AST and IgG below the upper limit of normal
Time frame: 24 weeks
Proportion of patients with partial response
defined as decrease of AST and ALT, but no normalization
Time frame: 52 weeks
Proportion of patients with insufficient treatment response
less than 25% reduction in ALT after 6 and 12 months treatment
Time frame: 52 weeks
Dose reduction of prednisone
Difference between dose at inclusion and dose at the end of study
Time frame: 52 weeks
Cessation rate of prednisone
The number of patients able to completely withdraw from corticosteroids
Time frame: 52 weeks
Change of AST
at 6 and 12 months versus baseline and between groups at the same time points
Time frame: 24 and 52 weeks
Change of ALT
at 6 and 12 months versus baseline and between groups at the same time points
Time frame: 24 and 52 weeks
Change of IgG
at 6 and 12 months versus baseline and between groups at the same time points
Time frame: 24 and 52 weeks
Liver function
Total bilirubin, albumin, INR and MELD-score after 6 and 12 months between groups
Time frame: 24 and 52 weeks
Fibrosis
Liver stiffness as measured by elastography and blood fibrosis markers (ELF)
Time frame: 52 weeks
Influence of liver disease on the quality of life
using the validated liver disease symptom index (LDSI)
Time frame: 52 weeks
Treatment effect on health status
using the validated EQ5D
Time frame: 52 weeks
Cost-effectiveness based on empiric data obtained by this study.
Economic evaluation including a cost-effectiveness evaluation
Time frame: 52 weeks
Cost-effectiveness from a societal perspective
Economic evaluation including a cost-utility evaluation (costs per QALY)
Time frame: 52 weeks
Bart van Hoek
CONTACT
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