ce) inhibitors are used concomitantly because sodium loss may reduce the renal clearance of lithium and increase serum lithium levels with risk of lithium toxicity. when such combinations are used, the lithium dosage may need to be decreased, and more frequent monitoring of lithium plasma levels is recommended. non-steroidal anti-inflammatory drugs (nsaids): lithium levels should be closely monitored when patients initiate or discontinue nsaid use. in some cases, lithium toxicity has resulted from interactions between an nsaid and lithium. indomethacin and piroxicam have been reported to increase significantly steady-state plasma lithium concentrations. there is also evidence that other nonsteroidal anti-inflammatory agents, including the selective cyclooxygenase-2 (cox-2) inhibitors, have the same effect. in a study conducted in healthy subjects, mean steady-state lithium plasma levels increased approximately 17% in subjects receiving lithium 450 mg bid with celecoxib 200 mg bid as compared to subjects receiving lithium alone.

such patients should be carefully managed to avoid dehydration with resulting lithium retention and toxicity. this condition is usually reversible when lithium is discontinued. morphologic changes with glomerular and interstitial fibrosis and nephron-atrophy have been reported in patients on chronic lithium therapy. morphologic changes have also been seen in bipolar patients never exposed to lithium. the relationship between renal functional and morphologic changes and their association with lithium therapy has not been established. when kidney function is assessed, for baseline data prior to starting lithium therapy or thereafter, routine urinalysis and other tests may be used to evaluate tubular function (e.g., urine specific gravity or osmolality following a period of water deprivation, or 24-hour urine volume) and glomerular function (e.g., serum creatinine or creatinine clearance). during lithium therapy, progressive or sudden changes in renal function, even within the normal range, indicate the need for reevaluation of treatment. lithium toxicity is closely related to serum lithium levels, and can occur at doses close to therapeutic levels (see dosage and administration ).

a temporary reduction or cessation of medication. previously existing underlying thyroid disorders do not necessarily constitute a contraindication to lithium treatment; where hypothyroidism exists, careful monitoring of thyroid function during lithium stabilization and maintenance allows for correction of changing thyroid parameters, if any. where hypothyroidism occurs during lithium stabilization and maintenance, supplemental thyroid treatment may be used.

um levels of 1.0 to 1.5 meq/ml. elderly patients often respond to reduced dosage, and may exhibit signs of toxicity at serum levels ordinarily tolerated by other patients. n.b. blood samples for serum lithium determination should be drawn immediately prior to the next dose when lithium concentrations are relatively stable (i.e., 8 to 12 hours after the previous dose). total reliance must not be placed on serum levels alone. accurate patient evaluation requires both clinical and laboratory analysis.

g the first few days of lithium administration. these side effects are an inconvenience rather than a disabling condition, and usually subside with continued treatment or a temporary reduction or cessation of dosage. if persistent, a cessation of dosage is indicated. the following adverse reactions have been reported and do not appear to be directly related to serum lithium levels. neuromuscular: tremor, muscle hyperirritability (fasciculations, twitching, clonic movements of whole limbs), ataxia, choreo-athetotic movements, hyperactive deep tendon reflexes. central nervous system: blackout spells, epileptiform seizures, slurred speech, dizziness, vertigo, incontinence of urine or feces, somnolence, psychomotor retardation, restlessness, confusion, stupor, coma, acute dystonia, downbeat nystagmus. cardiovascular: cardiac arrhythmia, hypotension, peripheral circulatory collapse, sinus node dysfunction with severe bradycardia (which may result in syncope). neurological: cases of pseudotumor cerebri (increased intracranial pressure and papilledema) have been reported with lithium use. if undetected, this condition may result in enlargement of the blind spot, constriction of visual fields and eventual blindness due to optic atrophy. lithium should be discontinued, if clinically possible, if this syndrome occurs. gastrointestinal: anorexia, nausea, vomiting, diarrhea. genitourinary: albuminuria, oliguria, polyuria, glycosuria. dermatologic: drying and thinning of hair, anesthesia of skin, chronic folliculitis, xerosis cutis, alopecia and exacerbation of psoriasis. autonomic nervous system: blurred vision, dry mouth. thyroid abnormalities: euthyroid goiter and/or hypothyroidism (including myxedema) accompanied by lower t 3 and t 4 . iodine 131 uptake may be elevated. (see precautions ). paradoxically, rare cases of hyperthyroidism have been reported. eeg changes: diffuse slowing, widening of frequency spectrum, potentiation and disorganization of background rhythm. ekg changes: reversible flattening, isoelectricity or inversion of t-waves. miscellaneous: fatigue, lethargy, transient scotomata, dehydration, weight loss, tendency to sleep. miscellaneous reactions unrelated to dosage are: transient electroencephalographic and electrocardiographic changes, leucocytosis, headache, diffuse non-toxic goiter with or without hypothyroidism, transient hyperglycemia, generalized pruritis with or without rash, cutaneous ulcers, albuminuria, worsening of organic brain syndromes, excessive weight gain, edematous swelling of ankles or wrists, and thirst or polyuria, sometimes resembling diabetes insipidus, and metallic taste. a single report has been received of the development of painful discoloration of fingers and toes and coldness of the extremities within one day of the starting of treatment of lithium. the mechanism through which these symptoms (resembling raynaud’s syndrome) developed is not known. recovery followed discontinuance.

ce) inhibitors are used concomitantly because sodium loss may reduce the renal clearance of lithium and increase serum lithium levels with risk of lithium toxicity. when such combinations are used, the lithium dosage may need to be decreased, and more frequent monitoring of lithium plasma levels is recommended. non-steroidal anti-inflammatory drugs (nsaids): lithium levels should be closely monitored when patients initiate or discontinue nsaid use. in some cases, lithium toxicity has resulted from interactions between an nsaid and lithium. indomethacin and piroxicam have been reported to increase significantly steady-state plasma lithium concentrations. there is also evidence that other nonsteroidal anti-inflammatory agents, including the selective cyclooxygenase-2 (cox-2) inhibitors, have the same effect. in a study conducted in healthy subjects, mean steady-state lithium plasma levels increased approximately 17% in subjects receiving lithium 450 mg bid with celecoxib 200 mg bid as compared to subjects receiving lithium alone.