Nunn Caroline, Langenegger Daniel, Hurth Konstanze, Schmidt Kerstin, Fehlmann Dominique, Hoyer Daniel
Nervous System Research, Novartis Pharma AG, CH-4002, Basel, Switzerland.
Eur J Pharmacol. 2003 Apr 4;465(3):211-8. doi: 10.1016/s0014-2999(03)01482-1.
The availability of antagonist ligands for somatostatin receptors is very limited, with those that are available often displaying agonist properties or limited receptor subtype selectivity. Hay et al. [Bioorg. Med. Chem. Lett. 11 (2001) 2731] recently described the development of small-molecule somatostatin receptor subtype 2 (sst(2)) selective compounds. This study investigates the binding affinity and functional characteristics of two of those antagonists (2 and 3) and the agonist compound, from which they were derived (1). In radioligand binding studies using the agonist radioligands [125I][Tyr(11)]SRIF-14 (Ala-Gly-c[Cys-Lys-Asn-Phe-Phe-Trp-Lys-Thr-(125I-Tyr)-Thr-Ser-Cys]-OH), [125I]LTT-SRIF-28 ([Leu(8),DTrp(22),125I-Tyr(25)]SRIF-28; Ser-Ala-Asn-Ser-Asn-Pro-Ala-Leu-Ala-Pro-Arg-Glu-Arg-Lys-Ala-Gly-c[Cys-Lys-Asn-Phe-Phe-DTrp-Lys-Thr-(125I-Tyr)-Thr-Ser-Cys]-OH), [125I]CGP 23996 (c[Lys-Asu-Phe-Phe-Trp-Lys-Thr-(125I-Tyr)-Thr-Ser]), [125I][Tyr(3)]octreotide (DPhe-c[Cys-(125I-Tyr)-DTrp-Lys-Thr-Cys]-Thr-OH) and [125I][Tyr(10)]cortistatin-14 (Pro-c[Cys-Lys-Asn-Phe-Phe-Trp-Lys-Thr-(125I-Tyr)-Ser-Ser-Cys]-Lys) at human recombinant somatostatin receptors expressed in Chinese hamster lung fibroblast (CCL39) cells and native rat cortex, the compounds bound with high affinity (pK(d) 6.8-9.7) and selectivity to human sst(2) receptors. Some affinity was also observed for sst(5) labelled by [125I][Tyr(3)]octreotide and [125I]CGP 23996. In functional studies at human sst(2) receptors expressed in Chinese hamster ovary (CHO) cells, both the agonist 1 and the two putative antagonists 2 and 3 concentration dependently inhibited forskolin-stimulated adenylate cyclase and stimulated luciferase reporter gene expression, with similar efficacy to the natural ligand somatotropin release inhibiting factor (SRIF)-14. Compound 1 had similar potency to SRIF-14, which was in the nanomolar range, whereas 2 and 3 were 10-100-fold less potent. The intrinsic activity of 2 and 3 was too high to allow antagonist studies to be carried out. In conclusion, in contrast to previous findings, all three compounds are potent agonists at recombinant human sst(2) receptors.
生长抑素受体拮抗剂配体的可用性非常有限,现有的那些配体常常表现出激动剂特性或有限的受体亚型选择性。Hay等人[《生物有机与药物化学快报》11 (2001) 2731]最近描述了小分子生长抑素受体2型(sst(2))选择性化合物的研发情况。本研究考察了其中两种拮抗剂(2和3)以及它们所衍生自的激动剂化合物(1)的结合亲和力和功能特性。在使用激动剂放射性配体[125I][Tyr(11)]SRIF - 14(Ala - Gly - c[Cys - Lys - Asn - Phe - Phe - Trp - Lys - Thr - (125I - Tyr) - Thr - Ser - Cys] - OH)、[125I]LTT - SRIF - 28([Leu(8),DTrp(22),125I - Tyr(25)]SRIF - 28;Ser - Ala - Asn - Ser - Asn - Pro - Ala - Leu - Ala - Pro - Arg - Glu - Arg - Lys - Ala - Gly - c[Cys - Lys - Asn - Phe - Phe - DTrp - Lys - Thr - (125I - Tyr) - Thr - Ser - Cys] - OH)、[125I]CGP 23996(c[Lys - Asu - Phe - Phe - Trp - Lys - Thr - (125I - Tyr) - Thr - Ser])、[125I][Tyr(3)]奥曲肽(DPhe - c[Cys - (125I - Tyr) - DTrp - Lys - Thr - Cys] - Thr - OH)和[125I][Tyr(10)]皮质抑素 - 14(Pro - c[Cys - Lys - Asn - Phe - Phe - Trp - Lys - Thr - (125I - Tyr) - Ser - Ser - Cys] - Lys)在中国仓鼠肺成纤维细胞(CCL39)中表达的人重组生长抑素受体以及天然大鼠皮质上进行的放射性配体结合研究中,这些化合物与人类sst(2)受体具有高亲和力(pK(d) 6.8 - 9.7)和选择性。对于用[125I][Tyr(3)]奥曲肽和[125I]CGP 23996标记的sst(5)也观察到了一些亲和力。在对中国仓鼠卵巢(CHO)细胞中表达的人类sst(2)受体进行的功能研究中,激动剂1以及两种假定的拮抗剂2和3均浓度依赖性地抑制福斯高林刺激的腺苷酸环化酶并刺激荧光素酶报告基因表达,并具有与天然配体生长激素释放抑制因子(SRIF) - 14相似的效力。化合物1与SRIF - 14具有相似的效力,处于纳摩尔范围,而2和3的效力则低10 - 100倍。2和3的内在活性过高,无法进行拮抗剂研究。总之,与先前的发现相反,所有这三种化合物在重组人sst(2)受体上都是强效激动剂。
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