Autoimmune Hepatitis Clinical Trial
Official title:
Identification of Biomarkers That Help to Predict Success of Immunosuppression Withdrawal in Patients With Type 1 Autoimmune Hepatitis
Autoimmune hepatitis (AIH) is an inflammatory, chronic and recurrent liver disease of unknown
etiology that can lead to cirrhosis or acute liver failure. It is a rare disease affecting 16
cases every 100,000 persons in Europe, mainly in women in every age group. It is
characteristic the presence of high levels of aminotransferases, hypergammaglobulinemia and
high titres of autoantibodies, as well as interface hepatitis in the biopsy.
Due to the autoimmune etiology of AIH, treatment is based on immunosuppressive strategies,
mainly prednisone and azathioprine regimens which make possible to achieve remission in
approximately 75% of cases with moderate or severe hepatocellular inflammation.
Remission is defined as a normalization in aminotransferases, immunoglobulin G (IgG) and
resolution histological inflammation (this last one comes after biochemical remission). It
has also been observed that there is a restoration in number and function of Tregs after
achieving remission.
The rates of recurrence after withdrawing it varies from 30-87% depending on the studies and
their follow-up. It is usual to maintain treatment indefinitely in clinical practice. This
strategy implies maintaining treatment for long periods of time in patients that could be
available to maintain sustained remission, exposing them to adverse effects. From all these,
we think it is important to be able to identify patients who will be able to maintain
biochemical and histological remission without immunosuppression (IS), which still is not
known in this disease's management.
Some observational and retrospective studies have identified some parameters that could imply
a higher risk of recurrence after stopping treatment such as high levels of aminotransferases
and IgG, less time of remission before withdrawal (specifically less than 2 years) or
presence of interface hepatitis in a biopsy prior discontinuation of treatment. However, the
accuracy of these parameters is low and as a result, management of this disease has not
changed much over the past decades, still having patients under prolonged treatment
unnecessarily.
For the previously mentioned reasons, there is a need to identify new biomarkers that allow
clinicians selecting patients with AIH in whom treatment could be stopped avoiding its costs
and adverse effects. At the same time, it would help to understand the immunopathogenesis of
AIH and identification of new therapeutic targets.
Study design: This is a prospective not controlled, not randomized, unicentric study to
establish predictive biomarkers for a safe and effective treatment withdrawal in patients
with type 1 AIH.
Length of the study: Screening is expected to take a year. Treatment withdrawal will be done
gradually over a period of 6 months and there will be a follow-up of 18 months.
Sample size: The rate of recurrence has been around 36% in some studies. However, this rate
is uncertain and it depends on the studied population and the afterwards follow-up. That is
why investigators have calculated the sample size with the confidence interval of this rate
and a 10% precision which was of 87 patients. Expecting 10% of losses, the final sample size
is 96 patients.
Patients: Investigators will select 96 patients diagnosed with type 1 AIH with biochemical
remission of at least 3 years that are under immunosuppressive treatment followed in Hospital
Clinic Barcelona. Patients with type 2 AIH are excluded because of their proved high risk of
recurrence. Other inclusion and exclusion criteria are the following:
Treatment withdrawal: IS will be tapered gradually over a period of 6 months. Azathioprine
will be stopped during the first 3 months, reducing the dose 50% every month. Prednisone will
be tapered 2.5mg monthly until total withdrawal. During withdrawal and the first year after
stopping treatment patients will undergo laboratory tests on a monthly basis, afterwards,
follow-up will be done every 3 months until the end of the project.
Sustained remission: Patients that after stopping treatment maintain AST/ALT under 2 times
the upper normal limit.
Recurrence: Patients who do not fulfil previous criteria.
Data collection:
- Demographic variables: age, sex, time from diagnosis to treatment withdrawal, laboratory
information such as aminotransferases, gamma-glutamyl transferase (GGT), alkaline
phosphatase (AP) and autoantibodies.
- Histological sample at the moment of inclusion in which the following analysis will be
performed: usual staining techniques to evaluate the presence of portal inflammation,
interface hepatitis and fibrosis. Expression of a group of genes involved in liver
rejection (CXCL9, CXCL10, FoxP3, TK1, CD74, MMP9) will be evaluated with quantitative
polymerase chain reaction (qPCR) in RNA of the tissue samples cryopreserved at -80ºC.
Immunochemical staining to quantify the number of lymphocytes CD4+, CD8+ and Tregs.
- The following variables will be evaluated in blood samples collected at the inclusion
and in every follow-up visit:
- Flux cytometry: Frequency and characteristics of Tregs (CD4+, CD25+, CD127- and
FoxP3). The intracellular stain of CTLA-4 will be evaluated as well.
- Stimulation with interleukin 2 (IL2) to study Tregs response (measured by the
expression of pSTAT5 after 20minutes of stimulation and the afterwards production
of IL10).
- Autoantibodies titers: antinuclear autoantibodies (ANA), anti-smooth muscle
antibody(ASMA), anti-liver kidney microsome type 1 (antiLKM), anti-soluble liver
antigen (antiSLA) and immunoglobulins levels.
Statistical analysis: Categorical variables will be compared with Chi or Fisher tests.
Quantitative variables will be analyzed with non-parametric tests (Mann-Whitney for
independent samples and Wilcoxon for paired samples). To quantify the expression of genes in
blood and tissue sample the Ct of the gene will be normalized with the 3 "housekeeping" (18S,
HPRT, GAPDH) to generate the delta Ct. Results will be expressed as a relative expression of
the cDNA of the study and the calibrated sample. Differences of <0.05 will be considered as
statistically significant. Data analysis will be performed with Stata vs 15.1.
Ambition: Investigator's hypothesis is that those patients affected with type 1 AIH able to
maintain remission after treatment withdrawal will express distinctive serological and
histological biomarkers, making possible the identification of patients that could benefit
from stopping treatment in the future avoiding its costs and adverse effects. At the same
time, it would help to understand the immunopathogenesis of AIH and the identification of new
therapeutic targets. Therefore, changing the natural history of this disease where there has
been little advance in this field in the past decades.
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