G protein-coupled receptor interactions and modification of signalling involving the ghrelin receptor, GHSR1a.
Mitchell Ty RinguetJohn Barton FurnessSebastian George Barton FurnessPublished in: Journal of neuroendocrinology (2021)
The growth hormone secretagogue receptor 1a (GHSR1a) is intriguing because of its potential as a therapeutic target and its diverse molecular interactions. Initial studies of the receptor focused on the potential therapeutic ability for growth hormone (GH) release to reduce wasting in aging individuals, as well as food intake regulation for treatment of cachexia. Known roles of GHSR1a now extend to regulation of neurogenesis, learning and memory, gastrointestinal motility, glucose/lipid metabolism, the cardiovascular system, neuronal protection, motivational salience, and hedonic feeding. Ghrelin, the endogenous agonist of GHSR1a, is primarily located in the stomach and is absent from the central nervous system (CNS), including the spinal cord. However, ghrelin in the circulation does have access to a small number of CNS sites, including the arcuate nucleus, which is important in feeding control. At some sites, such as at somatotrophs, GHSR1a has high constitutive activity. Typically, ghrelin-dependent and constitutive GHSR1a activation occurs via Gα q/11 pathways. In vitro and in vivo data suggest that GHSR1a heterodimerises with multiple G protein-coupled receptors (GPCRs), including dopamine D1 and D2, serotonin 2C, orexin, oxytocin and melanocortin 3 receptors (MCR3), as well as the MCR3 accessory protein, MRAP2, providing possible mechanisms for its many physiological effects. In all cases, the receptor interaction changes downstream signalling and the responses to receptor agonists. This review discusses the signalling mechanisms of GHSR1a alone and in combination with other GPCRs, and explores the physiological consequences of GHSR1a coupling with other GPCRs.
Keyphrases
- growth hormone
- spinal cord
- escherichia coli
- multidrug resistant
- type diabetes
- spinal cord injury
- blood brain barrier
- binding protein
- metabolic syndrome
- fatty acid
- staphylococcus aureus
- blood pressure
- brain injury
- cerebrospinal fluid
- electronic health record
- blood glucose
- subarachnoid hemorrhage
- cerebral ischemia
- replacement therapy
- functional connectivity