2014
DOI: 10.1371/journal.pone.0092042
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Prolonged Calcitonin Receptor Signaling by Salmon, but Not Human Calcitonin, Reveals Ligand Bias

Abstract: Salmon calcitonin (sCT) and human calcitonin (hCT) are pharmacologically distinct. However, the reason for the differences is unclear. Here we analyze the differences between sCT and hCT on the human calcitonin receptor (CT(a)R) with respect to activation of cAMP signaling, β-arrestin recruitment, ligand binding kinetics and internalization. The study was conducted using mammalian cell lines heterologously expressing the human CT(a) receptor. CT(a)R downstream signaling was investigated with dose response prof… Show more

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Cited by 67 publications
(70 citation statements)
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“…Long residence time could drive sustained receptor activation through a single preformed stable binding event that persists after removal of unbound agonist (Fig. 1a), as has been implicated for a number of GPCR agonists [18,20,23]. In the simplest model, ligand binds to receptor to form ligand-receptor complexes and, in binding kinetic experiments, residence time is calculated at the reciprocal of the rate of dissociation (K off ) of these complexes (Eqn 1).…”
Section: Ligand Properties That Favor Persistent Receptor Interactionsmentioning
confidence: 97%
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“…Long residence time could drive sustained receptor activation through a single preformed stable binding event that persists after removal of unbound agonist (Fig. 1a), as has been implicated for a number of GPCR agonists [18,20,23]. In the simplest model, ligand binds to receptor to form ligand-receptor complexes and, in binding kinetic experiments, residence time is calculated at the reciprocal of the rate of dissociation (K off ) of these complexes (Eqn 1).…”
Section: Ligand Properties That Favor Persistent Receptor Interactionsmentioning
confidence: 97%
“…Using in vitro experiments this can be exhibited by 'wash-resistant' receptor activation, where signaling continues even after excess agonist is removed from the receptor by infinite dilution of the drug-containing buffer [8,9,[16][17][18][19][20][21][22]. It is anticipated that this could Thyroid-stimulating hormone SSIR >30 min a [9] Sphingosine-1 phosphate-1 SSIR; residence time and rebinding 300 min a Q6 [16,42] b2-adrenergic SSIR; exosite; membrane deposition >180 min a or >10 min b [25,27,43,44] Vasopressin-2 SSIR >40 min a [17] Glucagon-like peptide SSIR n.d. [37] Angiotensin-II SSIR >30 min b [45] Calcitonin a SSIR; residence time > 4320 min b [18] Serotonin 5-HT2B SSIR; residence time and rebinding >240 min a [19] GPR119…”
Section: Ligand Properties That Favor Persistent Receptor Interactionsmentioning
confidence: 99%
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“…Activation of ERK1/2 is clearly a pathway that amylin can use, but more work is needed to determine the precise circumstances under which this occurs and the mechanism involved. There has been no specific investigation of whether amylin-induced ERK activation is G protein dependent or arrestin mediated; however, the calcitonin receptor can recruit arrestin in response to human and salmon calcitonin (Andreassen et al, 2014). Amylin was recently reported to either increase or decrease ERK and Akt phosphorylation in dispersed islets, depending on the amylin and glucose concentration (Visa et al, 2015).…”
Section: Signalingmentioning
confidence: 99%