COMPARISON OF TREMOR RESPONSES TO ORALLY-ADMINISTERED ALBUTEROL AND TERBUTALINE

Abstract

This study was designed to compare the initial tremor response to 4.0 mg albuterol and 5.0 mg terbutaline orally administered and to study the question of tachyphylaxis by rechallenge after 3 wk of maintenance dosing. Twenty fasting patients with severe COPD in whom orally administered sympathomimetics were withheld for 2 wk were challenged with single doses of each drug in a crossover, randomized fashion 1 wk apart. Then after a further 3 wk of dosing 3 times a day of the second medication (10 patients received each medication), they were challenged once more 16 h after the last dose. Rest and postural tremor were measured at zero and 2 h using an accelerometer affixed to the finger, and measurements of subjective tremor, tremor power spectrum, plasma cyclic AMP and lactate, and forced vital capacity were also made. Postural tremor increased from 25.05 to 36.20 relative units for albuterol, an increase of 11.15 units, and from 24.90 to 57.70 units for terbutaline, an increase of 32.80 units (difference significant at p = 0.01). Plasma cyclic AMP (p < 0.01) and lactate (p = 0.05) increases were also less for albuterol, and the FEV1 and FVC responses, though about one third less, did not differ significantly. After 3 wk, mean base-line tremor for both drugs was elevated even 16 h after the last 3 times a day dosing (38.00 and 33.10) for albuterol and terbutaline (difference, NS), and responses were much less to the single tablet (3.40 and 9.10, respectively). Because current studies indicate albuterol plasma concentrations are at least as high as terbutaline concentrations after a single dose, and albuterol is more potent than terbutaline by inhalation (mg/mg), the reduced initial responses suggest a slower or less complete diffusion of albuterol into the effector compartments by the systemic route. This may be an advantage with respect to clinical acceptance. The elevated and essentially equal baseline values after 3 wk indicate accumulation of both drugs on a 3 times a day schedule, consistent with current pharmacokinetic studies.