Inactivation of the β-adrenergic receptor in cardiac muscle by dithiols

Abstract

The effect of sulfhydryl reagents on binding of the β-adrenergic antagonist (−)-[³H]dihydroalprenolol hydrochloride ((−)-[³H]DHA) to a microsomal fraction of rabbit ventricular muscle was studied. Incubation with the disulfide reducing agents dithiothreitol (DTT), 2-mercaptocthanol, and reduced glutathione resulted in loss of (−)-[³H]DHA binding. At 500 μM DTT, less than 50% of specific binding activity remained; at 100 mM, binding was completely eliminated. 2-Mercaptoethanol and reduced glutathione were less effective than DTT at inhibiting binding activity. The total binding capacity (B_max) decreased from 155.4 fmol mg⁻¹ of protein, in the absence of DTT, to 92.4 and 77.5 fmol mg⁻¹ at 0.25 and 0.7 mM DTT, respectively. The equilibrium dissociation constant (K_D) increased from 7.6 nM, in the absence of DTT, to 10.3 nM at 0.25 mM DTT and to 20.8 nM at 0.7 mM DTT. Thus, DTT-induced decline in (−)-[³H]DHA binding results from a decrease in both the number and affinity of membrane binding sites for the tracer. Receptors could be protected from DTT inactivation by preincubation with β-adrenergic ligands. Oxidants could not reverse inactivation, with the exception of o-iodosobenzoate which was only partially effective. Thus, the β-adrenergic receptor of rabbit ventricular muscle contains essential disulfide moietie(s) which can be inactivated by reducing thiols.