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Peptide aromatic interactions modulated by fluorinated residues: Synthesis structure and biological activity of Somatostatin analogs containing 3-(3′5′difluorophenyl)-alanine

机译:含氟残基调节的肽芳香相互作用:含3-(35-二氟苯基)-丙氨酸的生长抑素类似物的合成结构和生物学活性

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摘要

Somatostatin is a 14-residue peptide hormone that regulates the endocrine system by binding to five G-protein-coupled receptors (SSTR1–5). We have designed six new Somatostatin analogs with L-3-(3′,5′-difluorophenyl)-alanine (Dfp) as a substitute of Phe and studied the effect of an electron-poor aromatic ring in the network of aromatic interactions present in Somatostatin. Replacement of each of the Phe residues (positions 6, 7 and 11) by Dfp and use of a D-Trp8 yielded peptides whose main conformations could be characterized in aqueous solution by NMR. Receptor binding studies revealed that the analog with Dfp at position 7 displayed a remarkable affinity to SSTR2 and SSTR3. Analogs with Dfp at positions 6 or 11 displayed a π-π interaction with the Phe present at 11 or 6, respectively. Interestingly, these analogs, particularly [D-Trp8,L-Dfp11]-SRIF, showed high selectivity towards SSTR2, with a higher value than that of Octreotide and a similar one to that of native Somatostatin.
机译:生长抑素是一种14个残基的肽激素,通过与五个G蛋白偶联受体(SSTR1-5)结合来调节内分泌系统。我们设计了六个新的生长抑素类似物,用L-3-(3',5'-二氟苯基)-丙氨酸(Dfp)代替Phe,并研究了贫电子环在电子中存在的芳香相互作用网络中的作用。生长抑素。用Dfp取代每个Phe残基(6、7和11位),并使用D-Trp8产生的肽,其主要构象可以在NMR中表征。受体结合研究表明,Dfp在7位的类似物对SSTR2和SSTR3表现出显着的亲和力。 Dfp位于6或11位的类似物分别与存在于11或6位的Phe有π-π相互作用。有趣的是,这些类似物,特别是[D-Trp8,L-Dfp11] -SRIF,显示出对SSTR2的高选择性,其价值高于奥曲肽,且与天然生长抑素相似。

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