Novel high molecular weight albumin-conjugated angiotensin II activates β-arrestin and G-protein pathways

ConclusionsAddition of a high molecular weight molecule to Ang II reduced its AT1 receptor binding affinity, but did not significantly alter stimulation of aldosterone release or water consumption. The BSA-Ang II conjugate caused a greater saline appetite than Ang II suggesting that it may be a more efficacious agonist of this beta-arrestin-mediated response than Ang II. The higher potency calcium signaling response suggests that the G-protein-coupled responses predominate at physiological concentrations of Ang II, while the beta-arrestin response requires pathophysiological or pharmacological concentrations of Ang II to occur.

http://link.springer.com/10.1007/s12020-019-01930-z

Source: Endocrine - April 23, 2019 Category: Endocrinology Source Type: research

More News: Calcium | Endocrinology | Study