Beta-adrenoceptors in human alveolar macrophages isolated by elutriation.

Abstract

1. beta‐adrenoceptors on human alveolar macrophages obtained by bronchoalveolar lavage (BAL) from healthy smoking volunteers (n = 26) were characterized by studying cyclic AMP (cAMP) accumulation in intact macrophages evoked by adrenaline or isoprenaline, with or without appropriate antagonists and by radioligand binding to macrophage membranes, using [125I]‐iodopindolol (125IPIN) as beta‐adrenoceptor ligand. 2. In a second study, cAMP responses of alveolar macrophages to isoprenaline and PGE1 and of peripheral blood lymphocytes to isoprenaline were compared in smoking and non‐smoking healthy volunteers (n = 9 + 9), as our initial studies were performed in smokers, due to their higher cell yield. 3. BAL yielded 47 +/− 23 × 10(6) cells in smokers and 12 +/− 6 × 10(6) cells in non‐smokers with a recovery of 82 +/− 8% in the elutriation step (means +/− s.d.). The cell preparation consisted of 99.2 +/− 0.8% macrophages and their viability (trypan blue exclusion) was 97.5 +/− 5.2%. 4. Isoprenaline or adrenaline increased cAMP accumulation approximately 40‐fold with or without the phosphodiesterase inhibitor isobutylmethylxanthine (IBMX, 10(‐4) M), which enhanced basal and stimulated cAMP accumulation approximately five‐fold. Peak responses were seen after 2 min. EC50s for isoprenaline and adrenaline were 3‐5 × 10(‐7) M. Phentolamine did not alter responses to adrenaline, indicating absence of inhibitory alpha 2‐adrenoceptors. Propranolol inhibited isoprenaline induced cAMP accumulation stereoselectively; pD2‐values were 8.2 for (‐)‐ propranolol, 5.6 for atenolol and 7.5 for ICI 118,551, suggesting a predominance of beta 2‐adrenoceptors. 5. Specific 125IPIN binding to macrophage membranes was rapid and saturable. Non‐specific binding was determined in the presence of 1 microM (‐)‐propranolol. KD values were 71 +/− 7 pM and the density of specific binding sites was 36 +/− 3 fmol mg‐1 protein (three experiments on a membrane pool from 10 subjects; r values for Scatchard analyses = 0.98 +/− 0.01). Similar values were obtained when 200 microM isoprenaline (+ GTP) was used to assess non‐ specific binding. Competition experiments again showed stereoselectivity for propranolol and a predominance of beta 2‐ adrenoceptors, as judged by the displacement of specific 125IPIN binding by atenolol and ICI 118,551. 6. Macrophages from smokers responded with less marked cAMP accumulation upon stimulation with isoprenaline or PGE1 than did cells from non‐smokers (difference approximately 30%; P less than 0.05 for both agonists) in the presence of IBMX. Thus macrophages from smokers may produce less cAMP due to post‐receptor changes in responsiveness.(ABSTRACT TRUNCATED AT 400 WORDS)