强效假多肽炸弹蛋白样激动剂和拮抗剂。bombesin类似物的有序构象与受体活性的相关性。

J V Edwards, L R McLean, A C Wade, S R Eaton, E A Cashman, K A Hagaman, B O Fanger
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引用次数: 0

摘要

合成了类似炸弹素的假多肽,并对其理化性质和生物活性进行了研究。分别用psi[CH2S]和psi[CH2N(CH3)]修饰Bombesin和相关肽litorin的13-14位和8-9位。[Phe13 psi[CH2S]Leu14]bombesin和[Phe8 psi[CH2S]-Leu9]litorin与小鼠胰腺bombesin/胃泌素释放肽受体结合,具有相似的解离常数(Kd分别为3.9和3.4 nM)。通过将硫代亚甲基醚氧化为两种非对映异构体亚砜(异构体I, Kd = 1.6 nM和异构体II, Kd = 0.89 nM),提高了效能。进一步氧化砜降低了效价([Phe8 psi[CH2SO2]Leu9]litorin, Kd = 9.9 nM)。所有五种类似物都是受体拮抗剂,通过小鼠胰腺中磷脂酰肌醇的转换来确定。与这些肽主链取代相反,在8-9酰胺键位置的psi[CH2N(CH3)]产生激动剂。用CD和荧光光谱法将其与litorin (Kd = 0.1 nM)和[Leu9]litorin (Kd = 0.17 nM)进行比较。CD谱显示了TFE中所有肽的有序构象。根据两性离子洗涤剂中肽的荧光光谱对ph值的依赖性,确定了两个可滴定基团(pKa = 6.3和8.5)。在激动剂类似物中发现较低的pKa,但在含有psi [CH2S]的拮抗剂中没有发现。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Potent pseudopeptide bombesin-like agonists and antagonists. Correlation of ordered conformation of bombesin analogs to receptor activity.

Bombesin-like pseudopeptides have been synthesized, and certain physicochemical properties and biological activities have been examined. Bombesin and the related peptide litorin were modified at positions 13-14 and 8-9, respectively, with psi[CH2S] and psi[CH2N(CH3)]. [Phe13 psi[CH2S]Leu14]bombesin and [Phe8 psi[CH2S]-Leu9]litorin bound to the murine pancreatic bombesin/gastrin releasing peptide receptor with similar dissociation constants (Kd = 3.9 and 3.4 nM, respectively). Increased potency was achieved by oxidation of the thiomethylene ether to two diastereomeric sulfoxides (isomer I, Kd = 1.6 nM and isomer II, Kd = 0.89 nM. Further oxidation to the sulfone decreased potency ([Phe8 psi[CH2SO2]Leu9]litorin, Kd = 9.9 nM). All five analogs were receptor antagonists as determined by phosphatidylinositol turnover in murine pancreas. In contrast to these peptide backbone substitutions, a psi[CH2N(CH3)] at the 8-9 amide bond position resulted in an agonist. The analogs were compared with those of litorin (Kd = 0.1 nM) and [Leu9]litorin (Kd = 0.17 nM) by CD and fluorescence spectroscopy. The CD spectra demonstrated ordered conformation for all the peptides in TFE. Different conformations corresponding to agonist and antagonist peptides were suggested by CD. Based on the pH-dependence of the fluorescence spectra of the peptides in a zwitterionic detergent, two titratable groups were identified (pKa = 6.3 and 8.5). The lower pKa is found in the agonist analogs but not in the psi [CH2S]-containing antagonist.

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