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线虫FMRF酰胺相关肽KNEFIRFamide(AF1)对猪蛔虫肌肉的构效关系

Structure-activity relationships of KNEFIRFamide (AF1), a nematode FMRFamide-related peptide, on Ascaris suum muscle.

作者信息

Bowman J W, Friedman A R, Thompson D P, Ichhpurani A K, Kellman M F, Marks N, Maule A G, Geary T G

机构信息

Pharmacia & Upjohn, Inc., Kalamazoo, MI 49001-0199, USA.

出版信息

Peptides. 1996;17(3):381-7. doi: 10.1016/0196-9781(96)00007-1.

DOI:10.1016/0196-9781(96)00007-1
PMID:8735963
Abstract

Analogues of KNEFIRFamide (Lys-Asn-Glu-Phe-Ile-Arg-Phe-NH2; AF1), an FMRFamide-related peptide (FaRP) originally isolated from Ascaris suum, were characterized in an A. suum muscle tension assay. AF1 had biphasic effects on this preparation, inducing a brief relaxation followed by excitation and spastic paralysis. Activity of AF1 in this assay was eliminated by N-terminal deletions and by deamidation of the carboxy-terminus. The potency of AF1 was greatly reduced by alanine substitution for any residue. Peptides that retained activity did not show the biphasic response observed with AF1, suggesting that the inhibitory and excitatory phases seen with AF1 may be due to activation of distinct receptors. The basis for the marked differences in potency observed between AF1 and the structurally related nematode FaRP, AF2 (KHEYLRFamide) was also tested. AF2 is approximately 1000-fold more potent than AF1 in this assay, but has physiological effects that are otherwise indistinguishable. KNEYIRFamide and KNEFLRFamide induced characteristic AF1/AF2 responses, but were much less potent than the native peptides. In contrast, KHEYIRFamide resembled AF1 in potency and pattern of responses. These data suggest that AF1 and AF2 act at distinct receptors, and hypothesis supported by the observation that KNEFIAFamide antagonized the effects of AF1 but not of AF2.

摘要

KNEFIRFamide(Lys-Asn-Glu-Phe-Ile-Arg-Phe-NH2;AF1)是一种最初从猪蛔虫中分离出的FMRF酰胺相关肽(FaRP),其类似物在猪蛔虫肌肉张力测定中得到了表征。AF1对该制剂有双相作用,先引起短暂松弛,随后是兴奋和痉挛性麻痹。在该测定中,AF1的活性通过N端缺失和羧基末端的脱酰胺作用而消除。用丙氨酸替代任何残基都会大大降低AF1的效力。保留活性的肽没有显示出与AF1观察到的双相反应,这表明AF1所见的抑制和兴奋阶段可能是由于不同受体的激活。还测试了AF1与结构相关的线虫FaRP AF2(KHEYLRFamide)之间效力显著差异的基础。在该测定中,AF2的效力比AF1高约1000倍,但其生理效应在其他方面难以区分。KNEYIRFamide和KNEFLRFamide诱导了特征性的AF1/AF2反应,但效力远低于天然肽。相比之下,KHEYIRFamide在效力和反应模式上与AF1相似。这些数据表明AF1和AF2作用于不同的受体,KNEFIAFamide拮抗AF1的作用但不拮抗AF2的作用这一观察结果支持了这一假设。

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