Arginine vasopressin receptor 1B

Vasopressin V1b receptor (V1bR) also known as vasopressin 3 receptor (VPR3) or antidiuretic hormone receptor 1b is a is_associated_with::protein that in humans is encoded by the AVPR1B (arginine vasopressin receptor 1B) is_associated_with::gene.

V1bR acts as receptor for is_associated_with::arginine vasopressin. AVPR1B belongs to the subfamily of is_associated_with::G-protein coupled receptors. Its activity is mediated by G proteins which stimulate a is_associated_with::phosphatidylinositol-is_associated_with::calcium second messenger system.It is a major contributor to homeostasis and the control of water, glucose, and salts in the blood. Arginine vasopressin has four receptors, each of which are located in different tissues and have specific functions. AVPR1b is a g-protein coupled pituitary receptor that has only recently been characterized because of its rarity.

It has been found that the 420-amino-acid sequence of the AVPR1B receptor shared the most overall similarities with the AVP1A, AVP2 and oxytocin receptors. AVPR1B maps to chromosome region 1q32 and is a member of the vasopressin/oxytocin family subfamily.

Tissue distribution
AVPR1B was initially described as a novel vasopressin receptor located in the is_associated_with::anterior pituitary, where it stimulates is_associated_with::ACTH release. Subsequent studies have shown that it is also present in the brain.

Behavioral
Inactivation of the Avpr1b gene in mice (knockout) produces mice with greatly reduced aggression and a reduced ability to recognize recently investigated mice. Interestingly, is_associated_with::defensive behaviour and predatory behaviours appear normal in these knockout mice, but there is evidence that social motivation or awareness is reduced. The AVPR1B antagonist, SSR149415, has been shown to have anti-aggressive actions in hamsters and anti-depressant- and anxiety (anxiolytic)-like behaviors in rats. A is_associated_with::single nucleotide polymorphism (SNP) has been associated with susceptibility to depression in man.

Metabolic
Various stress-induced elevations of ACTH are blunted in the Avpr1b knockout mouse.

Oncology
AVPR1B is expressed at high levels in ACTH-secreting is_associated_with::pituitary adenomas as well as in is_associated_with::bronchial carcinoids responsible for the is_associated_with::ectopic ACTH syndrome.

Ligands
is_associated_with::Nelivaptan (SSR149415) and D-[Leu4-Lys8]-vasopressin are a specific antagonist and is_associated_with::agonist for the vasopressin 1b receptor, respectively.

Function
AVPR1B is found in different parts of the body and thus has several influences and regulatory actions. Arginine vasopressin influences several symptoms related to affective disorders including significant memory processes, pain sensitivity, synchronization of biological rhythms and the timing and quality of REM sleep. Studies have shown that AVPR1B deficiencies produce behavioral changes that can be reversed when the peptide is replaced. These effects are expressed through contact with specific plasma membrane receptors. AVPR1B is responsible for fueling the effects of vasopressin on ACTH release. This interaction takes place as Arginine Vasopressin works with corticotropin releasing hormone to stimulate the pituitary gland to secrete ACTH. AVPR1b is then responsible for mediating the stimulatory effect of vasopressin on ACTH release. Several G proteins are also involved in the signal transduction pathways linked with AVPR1B. These relationships depend on the level of receptor expression and concentration of vasopressin. For example, AVPR1B causes secretion of ACTH from the anterior pituitary cells in a dose-dependent relationship by activating protein kinase C via the Gq/11 protein.

Application
There have been several experiments which have studied these interactions further and revealed AVPR1B’s role in psychological disorders and regulatory functions. Halotypes of AVPR1B are associated with increased protective effects to recurrent major depression. AVPR1B has also been associated with higher cortisol responses to psychosocial stress in children with psychiatric disorders compared with carriers of glucocorticoid receptor gene. AVPR1b has also shown involvement in regulation of brain water content and cerebral edema. This was revealed as increased levels of AVPR1B mRNA on the choroid plexus were discovered as a result of increased plasma osmolality. The increase after a reduction of brain water content from salt water loading indicated AVPR1B’s role in the neuroendocrine feedback loop in maintaining normal central nervous system fluid balance.