Abstract
IV Abstract Relaxin has been known as a central hormone of pregnancy responsible for the dilatation of the birth canal since the beginning of the 20 century. Recent studies elucidated several new effects of relaxin such as regulation of vasotonus, renal function, and collagen turnover. In 2002, two G-protein-coupled receptors, LGR7 and LGR8, were identified as relaxin receptors. The present study shows for the first time that relaxin interacts as an agonist with glucocorticoid receptors (GR) in HeLaand THP-1-cells. Initially, co-immunoprecipitation experiments revealed binding of relaxin to glucocorticoid receptors. Treatment with relaxin led to translocation of relaxin and glucocorticoid receptors into the nucleus within 30 minutes. After stimulation with relaxin, cells transiently transfected with GRE-luciferase constructs demonstrated activation of glucocorticoid receptors. At the functional level, relaxin reduced – in GR-dependent manner TNFα-secretion of macrophages after stimulation with bacterial endotoxin. An increase of functionally active glucocorticoid receptors after incubation with relaxin was shown by PCR, western blots, and incorporation of H-labeled dexamethasone. All investigated effects of relaxin were abolished by co-treatment with the glucocorticoid receptor antagonist RU-486.
Published Version
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