Autoimmune Hepatitis Clinical Trial
Official title:
Association of Chloroquine and Prednisone as an Alternative Treatment for Autoimmune Hepatitis: a Randomized Trial
The gold-standard treatment of Autoimmune hepatitis (AIH), with prednisone alone or in conjunction with azathioprine can reach resolution of the disease in 70-80% of the cases in US. However, in Brazil the response to these treatments seems to be worse, approximately 35% in five years. Because of the side effects of the gold-standard treatment and the need for an alternative option for the no responsive patients, news drugs must be evaluated for this proposal. Chloroquine diphosphate is an antimalarial drug that has been used for the treatment of rheumatological diseases for at the least five decades. Chloroquine was used as a single drug for up to two years for the maintenance of AIH remission in an open study. There was a 6.49 greater chance of relapse in the historical controls when compared with patients treated with chloroquine (72.2% x 23.5%; p = 0.031). The aim of this study was to investigate whether chloroquine in conjunction with prednisone can be used as an alternative treatment of AIH in a randomized study, and to evaluate its side effects.
Autoimmune hepatitis (AIH) is a chronic disease with a progressive destruction of hepatic
parenchyma, leading to cirrhosis and high mortality in the absence of specific treatment. It
has been demonstrated that the treatment with corticosteroids and azathioprine provides
clinical and laboratory improvement, reduction of histological inflammatory activity on
liver biopsy and an increased survival.
Because of the side effects of the gold-standard treatment and the need for an alternative
option for the no responsive patients, news drugs must be evaluated for this proposal.
Chloroquine is a drug of the group of 4-aminoquinolines, synthetic derivatives of quinine
and constituent of the bark of the Cinchona tree. Chloroquine accumulates in tissues in
considerable amounts. In animals, from 200 to 700 times the plasma concentration can be
found in liver, spleen, kidneys and lungs. As a weak base, it accumulates intracellularly,
particularly in lysosomes with a consequent increase in pH within these organelles, which
could contribute to its toxicity. Lysosomal lamellar bodies are observed in tissues affected
by chloroquine, such as retina and neuromuscular system. Chloroquine inhibits the absorption
and the binding of mitochondrial calcium, alters the membrane permeability and the transport
of enzymes to the lysosomes. Apparently there are other mechanisms to explain its
anti-inflammatory action; such as the interference with the release of TNF from mononuclear
phagocytes by inhibiting gene expression and the down-regulation of TNF receptors, by
delaying their transport to the cellular surface. Due to these mechanisms of action,
chloroquine has anti-inflammatory activities and therefore is used in diseases such as
rheumatoid arthritis and systemic lupus erythematosus. In liver diseases, chloroquine was
used in patients with hepatitis B with normalization of the levels of aminotransferases and
of the prothrombin time during treatment and relapse after drug discontinuation. Chloroquine
was also evaluated in patients with porphyria cutanea tarda and despite the clinical and
biochemical improvement, liver biopsies remained unchanged after one year of treatment.
A previous pilot study was performed in our institution, and published in 2005, with
chloroquine diphosphate for the maintenance treatment of AIH. In this study, 14 patients
with a biochemical and histological remission were treated with chloroquine diphosphate 250
mg/day for at least 12 months or until disease recurrence, and compared with 18 historical
controls, which was held in discontinuation of treatment after remission. The chance of
relapse was 6.49 times higher in the historical controls when compared with patients in the
group treated with chloroquine (72.2% versus 23.5%, p = 0.031). The use of chloroquine was
safe in patients with liver cirrhosis without decompensation, and there were no serious
adverse events within two years of use.
The most common adverse effects of chloroquine are mild and transient such as
gastrointestinal symptoms, headache, dizziness, blurry vision and fatigue. The more severe
reactions described are itching, cardiovascular manifestations, dyskinesias, eye injuries,
neuromuscular disorders and hearing loss. Among the most feared adverse effects of
chloroquine, are the eye injuries, usually associated with chronic treatment. They may
consist of changes in the retina, lens, cornea and optic nerve. Usually they remain stable
after drug withdrawal, if the drug is discontinued in early stages. However, the retinal
damage can increase when found in advanced stages, and may progress even years after
cessation of chloroquine. It is believed that the chloroquine retinopathy can be prevented
or recognized in an early reversible stage with judicious use, appropriate doses and regular
ophthalmologic follow-up. It is recommended that the daily dose does not exceed 250 mg of
chloroquine diphosphate or 400 mg of hydroxychloroquine, and ophthalmologic evaluations are
carried out every 4 to 6 months. Despite the adverse effects and toxic reactions described
above, there is a consensus in most studies with chloroquine that it is a well tolerated
drug, provided that the appropriate dosage guidelines and regular eye examinations are
followed. With these cautions in mind, its use rarely causes serious side or irreversible
effects.
The aim of this study was to investigate whether chloroquine in conjunction with prednisone
can be used as an alternative treatment of AIH in a randomized study, and to evaluate its
side effects.
To be included patients had to satisfy the following criteria simultaneously: a diagnosis of
probable / definite AIH and the indication of treatment (according to the International AIH
Group), normal liver function and absence of clinical signs of decompensated liver disease
(ascites, hepatic encephalopathy, gastrointestinal bleeding and hepatocellular carcinoma).
For their enrollment, it is necessary that the patients are in accordance with the proposed
study, following the precepts of the Declaration of Helsinki. If patients refuse to
participate in the study, they will be treated following the traditional guidelines of our
service. Treatment will be discontinued in case of pregnancy, patient's desire, side-effects
or relapse of AIH.
Patients were randomized to receive azathioprine and prednisone or chloroquine and
prednisone. The alternative treatment, with chloroquine, was maintained unless it caused
major side-effects, no biochemical response or treatment failure. In this case, azathioprine
was introduced in association with prednisone. All patients had visits every 30 days during
the first six months with routine blood tests performed. After then, consultations were
every two months. All complaints were recorded. Every patient were treated by the doctors
responsible for the study, laboratory tests were performed in the Central Laboratory of the
hospital. All patients underwent to initial ophthalmologic evaluation followed by
six-monthly evaluations. The drug was withdrawal, if changes suggestive of retinopathy were
observed.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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