Tuberculosis Clinical Trial
Official title:
Study of Safety and Efficacy of Different Regimes of Reintroduction of Anti-TB Drugs in Antituberculosis Treatment Induced Hepatotoxicity
Purpose of the study is to evaluate the safety and efficacy of different re-introduction regimens in anti-TB drug induced liver damage. There is no consensus how best to treat such patients who developed drug induced liver damage.
Tuberculosis continues to be a major health problem in both the developing and developed
countries because of its resurgence in the immunosuppressed patients. Short course
chemotherapy containing isoniazid, rifampicin and pyrazinamide has proved to be highly
effective in the treatment of tuberculosis. One of its adverse effect is liver damage which
is the most common side effect leading to interruption of therapy.
There is lack of consensus guidelines for treatment of anti-TB drug induced liver damage
Whether the re-introduction should take place with all the drugs given together in full
doses (which reduces the chance of resistance and cost to the patient) or in a phased
manner. There is lack of studies which compared different regimens of re-introduction of
anti-TB drugs.
In this study, we will study three regimes of re-introduction of hepatotoxic
anti-tuberculosis drugs (Rifampicin, Isoniazide, Pyrazinamide). These are potent
anti-tuberculosis medications and need to be restarted in patients who developed liver
toxicities attributed to these medications and became normal when these medicines were
stopped. At the time of re-introduction the patients will be randomized in 3 groups.
- First group will receive Isoniazide(5mg/kg/day), Rifampicin(10mg/kg/day) and
Pyrazinamide(25mg/kg/day) in full doses on day 1 and continued further.
- second group will receive Rifampicin(10mg/kg/day) in full dose on day 1 and continued,
Isoniazide(5mg/kg/day)in full dose on day 8 and continued, Pyrazinamide(25mg/kg/day)on
day 15 and continued.
- Third group will receive 100 mg/day of Isoniazide on day 1 which is gradually increased
to maximum dose (5mg/kg/day) by day 4 and continued. Rifampicin is introduced on day 8
in a dose of 150 mg/day which is gradually increased to maximum dose (10mg/kg/day) by
day 11 and continued. Pyrazinamide is introduced on day 15 in a dose of 500mg/day which
is gradually increased to maximum dose (25mg/kg/day) by day 18 and continued.
All the three groups will be monitored for three months by analyzing weekly liver function
tests. Any difference in the morbidity, deranged liver function or any other adverse effects
will be monitored and treated appropriately.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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