IngentaConnect Effects of rac-albuterol on arterial blood gases in patients with...

Authors: Whale, Christopher I.; Sovani, Milind P.; Mortimer, Kevin; Oborne, Janet; Cooper, Sue; Harrison, Timothy W.; Tattersfield, Anne E.

Source: British Journal of Clinical Pharmacology, Volume 62, Number 2, August 2006 , pp. 153-157(5)

Publisher: Blackwell Publishing

Abstract:

Aims

Many patients with chronic obstructive pulmonary disease (COPD) are treated with high dose β₂-adrenoceptor agonists, which can increase ventilation/perfusion mismatching, and tremor and cardiac output, thereby increasing oxygen uptake and carbon dioxide output (VCO₂). Patients with severe COPD and hypercapnia may be unable to increase ventilation in response to increased VCO₂, in which case arterial carbon dioxide tension (P_aCO₂) may rise. Our aim was to determine whether high dose nebulized rac-albuterol could increase P_aCO₂ in patients with COPD, limited bronchodilator reversibilty and hypercapnia. Methods

We compared 10 mg and 400 µg rac-albuterol, given in two doses 1 h apart on nonconsecutive days, in a double-blind randomized crossover study in 14 patients with severe COPD. P_aCO₂, arterial oxygen tension (P_aO₂) and heart rate were measured over 120 min and change from baseline was plotted against time to obtain an area under the curve. Results

Mean P_aCO₂ fell slightly over 120 min, with no difference between treatments (0.03 kPa h⁻¹ (95% confidence interval 0.02, 0.04)) and only three subjects had an increase in P_aCO₂ after high dose rac-albuterol. High dose rac-albuterol caused a greater fall in P_aO₂[0.1 kPa h⁻¹ (95% confidence interval 0, 0.2)] and increase in heart rate than the low dose, although the differences were small. Conclusions

Under stable conditions most subjects with severe COPD and hypercapnia will have a fall in P_aCO₂ and P_aO₂ following 10 mg rac-albuterol, suggesting that they maintain capacity to respond to any increase in VCO₂ and prevent a rise in P_aCO₂.

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Effects of rac-albuterol on arterial blood gases in patients with stable hypercapnic chronic obstructive pulmonary disease