Summary
In vitro incubation studies with bovine parathyroid gland slices compared the relative responsiveness
of parathyroid hormone (PTH) secretion to isoproterenol, epinephrine or norepinephrine.
Isoproterenol was the most potent and norepinephrine the least potent of the three
stimuli, suggesting a β2 type of an adrenergic response. However in this in vitro system, tazalol, a selective β1 adrenergic agonist significantly stimulated PTH secretion, whereas terbutaline, a
selective β2 agonist had no effect. In addition, practolol, a selective β1 adrenergic antagonist blocked isoproterenol- or tazolol-stimulated PTH secretion.
In vivo studies in normal human subjects showed that injection of the nonselective β agonist,
isoproterenol, (0.15 mg s.c.) significantly increased, whereas injection of the selective
β2 agonist, terbulatine (0.3 mg s.c.) had no effect on serum PTH levels. These latter
studies with putative selective β adrenergic agents suggest that the β adrenergic
receptor mediating PTH secretion is of the β1 type (in contrast to the studies above with nonselective agents). The studies suggest
that the β adrenergic receptor mediating PTH secretion apparently differs from the
classical β1 receptor described in the myocardium or the classical β2 receptor described in the bronchial smooth muscle.
Key-Words
Parathyroid Hormone
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β-Adrenergic Receptor
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Selective β-Adrenergic Agents
