Divergent structural requirements exist for calcitonin receptor binding specificity and adenylate cyclase activation
The basis of the high potency of salmon calcitonin (sCT) in radioligand binding competition and cAMP accumulation studies with cloned calcitonin (CT) receptors from rats, pigs, and humans was examined using two sets of CT analogues, i.e., chimeric sCT/human CT (hCT) analogues and analogues of sCT wi...
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Veröffentlicht in: | Molecular pharmacology 1995-04, Vol.47 (4), p.798-809 |
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Zusammenfassung: | The basis of the high potency of salmon calcitonin (sCT) in radioligand binding competition and cAMP accumulation studies
with cloned calcitonin (CT) receptors from rats, pigs, and humans was examined using two sets of CT analogues, i.e., chimeric
sCT/human CT (hCT) analogues and analogues of sCT with differing capacities to form an amphipathic alpha-helix. In competition
for 125I-sCT binding the following relative specificities were observed for the chimeric peptides: rat C1a CT receptor, sCT
> or = (1-16)hCT/(17-32)sCT (ACT-15) > (1-16)sCT/(17-32)hCT (ACT-27); rat C1b CT receptor, sCT > ACT-15 > ACT-27; hCT receptor,
sCT = ACT-15 > ACT-27; porcine CT receptor, sCT > ACT-27 > ACT-15. In contrast, in ligand-induced cAMP accumulation studies
the relative efficacies were as follows: rat C1a CT receptor, sCT = ACT-15 > ACT-27; rat C1b CT receptor, sCT = ACT-15 > ACT-27;
hCT receptor, sCT = ACT-15 > or = to ACT-27; porcine CT receptor, sCT = ACT-15 = ACT-27. The data demonstrate that residues
present in the carboxyl-terminal half of sCT are more important for binding competition with the rat C1a, rat C1b, and human
CT receptors, whereas residues in the amino-terminal half of sCT are more important for binding competition with the porcine
CT receptor. Carboxyl-terminal sCT residues are also important for full potency in adenylate cyclase activation with the rat
C1a and rat C1b CT receptors but are less important for activation via the hCT receptor. The disparity in the relative potencies
of the peptides in studies of binding competition and cAMP accumulation is suggestive of significant differences in the relative
affinities of the peptides for active and inactive conformations of the CT receptor. The use of sCT analogues with varying
capacities to form alpha-helices also revealed divergence in the responses of different receptors. This was most apparent
for the stimulation of cAMP production by the rat receptor isoforms C1a and C1b. In cells expressing the C1a receptor, the
helical analogues sCT and des-Ser2-sCT were equipotent with [Gly8]-des-Leu19-sCT and des-1-amino-[Ala1,7,Gly8]-des-Leu19 sCT,
analogues that have reduced or absent helical structure, respectively. In contrast, the nonhelical analogues were 100-1000-fold
less potent than sCT and des-Ser2-sCT at the C1b receptor. In general, reduction in the ability of sCT analogues to form helix
structures had a greater impact on the potency of the analogues in competition for 125I-sCT binding than in cAMP a |
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ISSN: | 0026-895X 1521-0111 |