ter after 12 weeks of treatment. trientine hydrochloride capsules are not indicated for treatment of biliary cirrhosis.

d be swallowed whole with water and should not be opened or chewed.

r established. to report suspected adverse reactions, contact dr. reddy’s laboratories, inc. at 1-888-375-3784 or fda at 1-800-fda-1088 or www.fda.gov/medwatch.

ration of trientine hydrochloride therapy was 48.7 months (range 2 to 164 months). thirty-four of the 41 patients improved, 4 had no change in clinical global response, 2 were lost to follow-up and one showed deterioration in clinical condition. one of the patients who improved while on therapy with trientine hydrochloride experienced a recurrence of the symptoms of systemic lupus erythematosus which had appeared originally during therapy with penicillamine. therapy with trientine hydrochloride was discontinued. no other adverse reactions, except iron deficiency, were noted among any of these 41 patients. one investigator treated 13 patients with trientine hydrochloride following their development of intolerance to d-penicillamine. retrospectively, he compared these patients to an additional group of 12 patients with wilson's disease who were both tolerant of and controlled with d-penicillamine therapy, but who failed to continue any copper chelation therapy. the mean age at onset of disease of the latter group was 12 years as compared to 21 years for the former group. the trientine hydrochloride group received d-penicillamine for an average of 4 years as compared to an average of 10 years for the non-treated group. various laboratory parameters showed changes in favor of the patients treated with trientine hydrochloride. free and total serum copper, sgot, and serum bilirubin all showed mean increases over baseline in the untreated group which were significantly larger than with the patients treated with trientine hydrochloride. in the 13 patients treated with trientine hydrochloride, previous symptoms and signs relating to d-penicillamine intolerance disappeared in 8 patients, improved in 4 patients, and remained unchanged in one patient. the neurological status in the trientine hydrochloride group was unchanged or improved over baseline, whereas in the untreated group, 6 patients remained unchanged and 6 worsened. kayser-fleischer rings improved significantly during trientine hydrochloride treatment. the clinical outcome of the two groups also differed markedly. of the 13 patients on therapy with trientine hydrochloride (mean duration of therapy 4.1 years; range 1 to 13 years), all were alive at the data cutoff date, and in the non-treated group (mean years with no therapy 2.7 years; range 3 months to 9 years), 9 of the 12 died of hepatic disease. chelating properties preclinical studies studies in animals have shown that trientine hydrochloride has cupriuretic activities in both normal and copper-loaded rats. in general, the effects of trientine hydrochloride on urinary copper excretion are similar to those of equimolar doses of penicillamine, although in one study they were significantly smaller. human studies renal clearance studies were carried out with penicillamine and trientine hydrochloride on separate occasions in selected patients treated with penicillamine for at least one year. six-hour excretion rates of copper were determined off treatment and after a single dose of 500 mg of penicillamine or 1.2 grams of trientine hydrochloride. the mean urinary excretion rates of copper were as follows: no. of patients single dose treatment basal excretion rate (μg cu + + /6hr) test-dose excretion rate (μg cu + + /6hr) 6 trientine, 1.2 g 19 234 4 penicillamine, 500 mg 17 320 in patients not previously treated with chelating agents, a similar comparison was made: no. of patients single dose treatment basal excretion rate (μg cu + + /6hr) test-dose excretion rate (μg cu + + /6hr) 8 trientine, 1.2 g 71 1326 7 penicillamine, 500 mg 68 1074 these results demonstrate that trientine hydrochloride is effective as a cupriuretic agent in patients with wilson's disease although on a molar basis it appears to be less potent or less effective than penicillamine. evidence from a radio-labelled copper study indicates that the different cupriuretic effect between these two drugs could be due to a difference in selectivity of the drugs for different copper pools within the body. pharmacokinetics data on the pharmacokinetics of trientine hydrochloride are not available. dosage adjustment recommendations are based upon clinical use of the drug (see dosage and administration).