s should be closely watched during initiation of thyroid replacement therapy. estrogen, oral contraceptives estrogens tend to increase serum thyroxine-binding globulin (tbg). in a patient with a nonfunctioning thyroid gland who is receiving thyroid replacement therapy, free levothyroxine may be decreased when estrogens are started thus increasing thyroid requirements. however, if the patient's thyroid gland has sufficient function, the decreased free thyroxine will result in a compensatory increase in thyroxine output by the thyroid. therefore, patients without a functioning thyroid gland who are on thyroid replacement therapy may need to increase their thyroid dose if estrogens or estrogen-containing oral contraceptives are given. tricyclic antidepressants use of thyroid products with imipramine and other tricyclic antidepressants may increase receptor sensitivity and enhance antidepressant activity; transient cardiac arrhythmias have been observed. thyroid hormone activity may also be enhanced. digitalis thyroid preparations may potentiate the toxic effects of digitalis. thyroid hormonal replacement increases metabolic rate, which requires an increase in digitalis dosage. ketamine when administered to patients on a thyroid preparation, this parenteral anesthetic may cause hypertension and tachycardia. use with caution and be prepared to treat hypertension, if necessary. vasopressors thyroid hormones increase the adrenergic effect of catecholamines such as epinephrine and norepinephrine. therefore, use of vasopressors in patients receiving thyroid hormone preparations may increase the risk of precipitating coronary insufficiency, especially in patients with coronary artery disease. therefore, use caution when administering vasopressors with liothyronine (t 3 ).

likelihood of occult cardiac disease. therefore, in patients with compromised cardiac function, use thyroid hormones in conjunction with careful cardiac monitoring. although the specific dosage of triostat depends upon individual circumstances, in patients with known or suspected cardiovascular disease the extremely rapid onset of action of triostat may warrant initiating therapy at a dose of 10 mcg to 20 mcg. (see dosage and administration .) myxedematous patients are very sensitive to thyroid hormones; dosage should be started at a low level and increased gradually as acute changes may precipitate adverse cardiovascular events. severe and prolonged hypothyroidism can lead to a decreased level of adrenocortical activity commensurate with the lowered metabolic state. when thyroid-replacement therapy is administered, the metabolism increases at a greater rate than adrenocortical activity. this can precipitate adrenocortical insufficiency. therefore, in severe and prolonged hypothyroidism, supplemental adrenocortical steroids may be necessary. in rare instances, the administration of thyroid hormone may precipitate a hyperthyroid state or may aggravate existing hyperthyroidism. extreme caution is advised when administering thyroid hormones with digitalis or vasopressors. (see precautions–drug interactions .) fluid therapy should be administered with great care to prevent cardiac decompensation. (see precautions–adjunctive therapy .)

ronine sodium is used in initiating oral therapy, the physician should bear in mind that there is a delay of several days in the onset of l-thyroxine activity and that intravenous therapy should be discontinued gradually.

tion of at least 65 mcg/day of intravenous liothyronine (t 3 ) in the initial days of therapy was associated with lower mortality. there is limited clinical experience with intravenous liothyronine (t 3 ) at total daily doses exceeding 100 mcg/day. no controlled clinical studies have been done with triostat . the following dosing guidelines have been derived from data analysis of myxedema coma/precoma case reports collected by smithkline beecham pharmaceuticals since 1963 and from scientific literature since 1956. an initial intravenous triostat dose ranging from 25 mcg to 50 mcg is recommended in the emergency treatment of myxedema coma/precoma in adults. in patients with known or suspected cardiovascular disease, an initial dose of 10 mcg to 20 mcg is suggested (see warnings ). however, both the initial dose and subsequent doses should be determined on the basis of continuous monitoring of the patient's clinical condition and response to triostat therapy. normally at least four hours should be allowed between doses to adequately assess therapeutic response and no more than 12 hours should elapse between doses to avoid fluctuations in hormone levels. caution should be exercised in adjusting the dose due to the potential of large changes to precipitate adverse cardiovascular events. review of the myxedema case reports indicates decreased mortality in patients receiving at least 65 mcg/day in the initial days of treatment. however, there is limited clinical experience at total daily doses above 100 mcg. see precautions–drug interactions for potential interactions between thyroid hormones and digitalis and vasopressors. pediatric use there is limited experience with triostat in the pediatric population. safety and effectiveness in pediatric patients have not been established. switching to oral therapy oral therapy should be resumed as soon as the clinical situation has been stabilized and the patient is able to take oral medication. when switching a patient to liothyronine sodium tablets from triostat , discontinue triostat , initiate oral therapy at a low dosage, and increase gradually according to the patient's response. if l-thyroxine rather than liothyronine sodium is used in initiating oral therapy, the physician should bear in mind that there is a delay of several days in the onset of l-thyroxine activity and that intravenous therapy should be discontinued gradually.

s should be closely watched during initiation of thyroid replacement therapy. estrogen, oral contraceptives estrogens tend to increase serum thyroxine-binding globulin (tbg). in a patient with a nonfunctioning thyroid gland who is receiving thyroid replacement therapy, free levothyroxine may be decreased when estrogens are started thus increasing thyroid requirements. however, if the patient's thyroid gland has sufficient function, the decreased free thyroxine will result in a compensatory increase in thyroxine output by the thyroid. therefore, patients without a functioning thyroid gland who are on thyroid replacement therapy may need to increase their thyroid dose if estrogens or estrogen-containing oral contraceptives are given. tricyclic antidepressants use of thyroid products with imipramine and other tricyclic antidepressants may increase receptor sensitivity and enhance antidepressant activity; transient cardiac arrhythmias have been observed. thyroid hormone activity may also be enhanced. digitalis thyroid preparations may potentiate the toxic effects of digitalis. thyroid hormonal replacement increases metabolic rate, which requires an increase in digitalis dosage. ketamine when administered to patients on a thyroid preparation, this parenteral anesthetic may cause hypertension and tachycardia. use with caution and be prepared to treat hypertension, if necessary. vasopressors thyroid hormones increase the adrenergic effect of catecholamines such as epinephrine and norepinephrine. therefore, use of vasopressors in patients receiving thyroid hormone preparations may increase the risk of precipitating coronary insufficiency, especially in patients with coronary artery disease. therefore, use caution when administering vasopressors with liothyronine (t 3 ).

liver and kidney. a second pathway of t 4 to t 3 conversion occurs via a ptu-insensitive 5'-deiodinase located primarily in the pituitary and central nervous system. the prohormone t 4 must be converted to t 3 in the body before it can exert biological effects. during periods of illness or stress, this conversion is often inhibited and can be diverted to the inactive reverse t 3 (rt 3 ) moiety. therefore, correction of the hypothyroid condition in patients with myxedema coma is facilitated by the parenteral administration of triiodothyronine (t 3 ). t 3 is bound much less firmly to serum binding proteins and therefore penetrates into the cells much more rapidly than t 4 . also, the binding of t 3 to a nuclear thyroid hormone receptor seems to initiate most of the effects of thyroid hormone in tissues. although most thyroid hormone analogs, both natural and synthetic, will bind to this protein, the affinity of t 3 for this receptor is roughly 10-fold higher than that of t 4 . thus, t 3 is the biologically active thyroid hormone. pharmacodynamics the clinical features of myxedema coma include depression of the cardiovascular, respiratory, gastrointestinal and central nervous systems, impaired diuresis, and hypothermia. administration of thyroid hormones reverses or attenuates these conditions. thyroid hormones increase heart rate, ventricular contractility and cardiac output, as well as decrease total systemic vascular resistance. they also increase the rate and depth of respiration, motilityof the gastrointestinal tract, rapidity of cerebration, and vasodilatation. thyroid hormones correct hypothermia by markedly increasing the basal metabolic rate, as well as the number and activity of mitochondria in almost all cells of the body. pharmacokinetics since liothyronine sodium (t 3 ) is not firmly bound to serum protein, it is readily available to body tissues. liothyronine sodium has a rapid cutoff of activity which permits quick dosage adjustment and facilitates control of the effects of overdosage, should they occur. the higher affinity of levothyroxine (t 4 ) as compared to triiodothyronine (t 3 ) for both thyroid-binding globulin and thyroid-binding prealbumin partially explains the higher serum levels and longer half-life of the former hormone. both protein-bound hormones exist in reverse equilibrium with minute amounts of free hormone, the latter accounting for the metabolic activity. t 4 is deiodinated to t 3 . a single dose of liothyronine sodium administered intravenously produces a detectable metabolic response in as little as two to four hours and a maximum therapeutic response within two days. however, no pharmacokinetic studies have been performed with intravenous liothyronine (t 3 ) in myxedema coma or precoma patients.

r precoma patients.