Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor

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Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor. / Sivertsen, B; Holliday, N; Madsen, A N; Holst, B.

In: British Journal of Pharmacology, Vol. 170, No. 7, 12.2013, p. 1349-62.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Sivertsen, B, Holliday, N, Madsen, AN & Holst, B 2013, 'Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor', British Journal of Pharmacology, vol. 170, no. 7, pp. 1349-62. https://doi.org/10.1111/bph.12361

APA

Sivertsen, B., Holliday, N., Madsen, A. N., & Holst, B. (2013). Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor. British Journal of Pharmacology, 170(7), 1349-62. https://doi.org/10.1111/bph.12361

Vancouver

Sivertsen B, Holliday N, Madsen AN, Holst B. Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor. British Journal of Pharmacology. 2013 Dec;170(7):1349-62. https://doi.org/10.1111/bph.12361

Author

Sivertsen, B ; Holliday, N ; Madsen, A N ; Holst, B. / Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor. In: British Journal of Pharmacology. 2013 ; Vol. 170, No. 7. pp. 1349-62.

Bibtex

@article{beae9d5394214243a23448ed0dbe0b03,
title = "Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor",
abstract = "UNLABELLED: The ghrelin receptor is a 7 transmembrane (7TM) receptor involved in a variety of physiological functions including growth hormone secretion, increased food intake and fat accumulation as well as modulation of reward and cognitive functions. Because of its important role in metabolism and energy expenditure, the ghrelin receptor has become an important therapeutic target for drug design and the development of anti-obesity compounds. However, none of the compounds developed so far have been approved for commercial use. Interestingly, the ghrelin receptor is able to signal through several different signalling pathways including Gαq , Gαi/o , Gα12/13 and arrestin recruitment. These multiple signalling pathways allow for functionally biased signalling, where one signalling pathway may be favoured over another either by selective ligands or through mutations in the receptor. In the present review, we have described how ligands and mutations in the 7TM receptor may bias the receptors to favour either one G-protein over another or to promote G-protein independent signalling pathways rather than G-protein-dependent pathways. For the ghrelin receptor, both agonist and inverse agonists have been demonstrated to signal more strongly through the Gαq -coupled pathway than the Gα12/13 -coupled pathway. Similarly a ligand that promotes Gαq coupling over Gαi coupling has been described and it has been suggested that several different active conformations of the receptor may exist dependent on the properties of the agonist. Importantly, ligands with such biased signalling properties may allow the development of drugs that selectively modulate only the therapeutically relevant physiological functions, thereby decreasing the risk of side effects.LINKED ARTICLES: This article is part of a themed section on Neuropeptides. To view the other articles in this section visit http://dx.doi.org/10.1111/bph.2013.170.issue-7.",
author = "B Sivertsen and N Holliday and Madsen, {A N} and B Holst",
note = "{\textcopyright} 2013 The British Pharmacological Society.",
year = "2013",
month = dec,
doi = "10.1111/bph.12361",
language = "English",
volume = "170",
pages = "1349--62",
journal = "British Journal of Pharmacology",
issn = "0007-1188",
publisher = "Wiley",
number = "7",

}

RIS

TY - JOUR

T1 - Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor

AU - Sivertsen, B

AU - Holliday, N

AU - Madsen, A N

AU - Holst, B

N1 - © 2013 The British Pharmacological Society.

PY - 2013/12

Y1 - 2013/12

N2 - UNLABELLED: The ghrelin receptor is a 7 transmembrane (7TM) receptor involved in a variety of physiological functions including growth hormone secretion, increased food intake and fat accumulation as well as modulation of reward and cognitive functions. Because of its important role in metabolism and energy expenditure, the ghrelin receptor has become an important therapeutic target for drug design and the development of anti-obesity compounds. However, none of the compounds developed so far have been approved for commercial use. Interestingly, the ghrelin receptor is able to signal through several different signalling pathways including Gαq , Gαi/o , Gα12/13 and arrestin recruitment. These multiple signalling pathways allow for functionally biased signalling, where one signalling pathway may be favoured over another either by selective ligands or through mutations in the receptor. In the present review, we have described how ligands and mutations in the 7TM receptor may bias the receptors to favour either one G-protein over another or to promote G-protein independent signalling pathways rather than G-protein-dependent pathways. For the ghrelin receptor, both agonist and inverse agonists have been demonstrated to signal more strongly through the Gαq -coupled pathway than the Gα12/13 -coupled pathway. Similarly a ligand that promotes Gαq coupling over Gαi coupling has been described and it has been suggested that several different active conformations of the receptor may exist dependent on the properties of the agonist. Importantly, ligands with such biased signalling properties may allow the development of drugs that selectively modulate only the therapeutically relevant physiological functions, thereby decreasing the risk of side effects.LINKED ARTICLES: This article is part of a themed section on Neuropeptides. To view the other articles in this section visit http://dx.doi.org/10.1111/bph.2013.170.issue-7.

AB - UNLABELLED: The ghrelin receptor is a 7 transmembrane (7TM) receptor involved in a variety of physiological functions including growth hormone secretion, increased food intake and fat accumulation as well as modulation of reward and cognitive functions. Because of its important role in metabolism and energy expenditure, the ghrelin receptor has become an important therapeutic target for drug design and the development of anti-obesity compounds. However, none of the compounds developed so far have been approved for commercial use. Interestingly, the ghrelin receptor is able to signal through several different signalling pathways including Gαq , Gαi/o , Gα12/13 and arrestin recruitment. These multiple signalling pathways allow for functionally biased signalling, where one signalling pathway may be favoured over another either by selective ligands or through mutations in the receptor. In the present review, we have described how ligands and mutations in the 7TM receptor may bias the receptors to favour either one G-protein over another or to promote G-protein independent signalling pathways rather than G-protein-dependent pathways. For the ghrelin receptor, both agonist and inverse agonists have been demonstrated to signal more strongly through the Gαq -coupled pathway than the Gα12/13 -coupled pathway. Similarly a ligand that promotes Gαq coupling over Gαi coupling has been described and it has been suggested that several different active conformations of the receptor may exist dependent on the properties of the agonist. Importantly, ligands with such biased signalling properties may allow the development of drugs that selectively modulate only the therapeutically relevant physiological functions, thereby decreasing the risk of side effects.LINKED ARTICLES: This article is part of a themed section on Neuropeptides. To view the other articles in this section visit http://dx.doi.org/10.1111/bph.2013.170.issue-7.

U2 - 10.1111/bph.12361

DO - 10.1111/bph.12361

M3 - Journal article

C2 - 24032557

VL - 170

SP - 1349

EP - 1362

JO - British Journal of Pharmacology

JF - British Journal of Pharmacology

SN - 0007-1188

IS - 7

ER -

ID: 119829219