人β-内啡肽。8、27位以及9或11位残基有修饰的类似物的合成及生物活性
Human beta-endorphin. Synthesis and biological activity of analogs with modification in residue positions 8, 27, and 9 or 11.
作者信息
Yamashiro D, Li C H, Westphal M
出版信息
Int J Pept Protein Res. 1984 Nov;24(5):520-4.
Three analogs of human beta-endorphin (beta h-ER) were synthesized by the solid-phase method: [Gln8,Trp27]-beta h-EP (I), [Gln8,Arg9,Trp27]-beta h-EP (II), and [Gln9,Arg11,Trp27]-beta h-EP (III). Radioreceptor binding assay with use of tritiated beta h-EP as primary ligand gave relative potencies as follows: beta h-EP, 100;I, 778;II, 467;III, 449. Relative potencies in an analgesic assay were: beta h-EP, 100;I, 114;II, 165;III, 83. The 8-11 segment of beta h-EP can tolerate a net increase in charge of +2 without diminishing analgesic potency. The substitution of Glu8 may be one of the more dependable means of designing beta-endorphin antagonists.
采用固相法合成了三种人β-内啡肽类似物(βh-ER):[谷氨酰胺8,色氨酸27]-βh-EP(I)、[谷氨酰胺8,精氨酸9,色氨酸27]-βh-EP(II)和[谷氨酰胺9,精氨酸11,色氨酸27]-βh-EP(III)。以氚标记的βh-EP作为主要配体进行放射受体结合试验,得到的相对效价如下:βh-EP为100;I为778;II为467;III为449。镇痛试验中的相对效价为:βh-EP为100;I为114;II为165;III为83。βh-EP的8-11片段可以耐受净电荷增加+2而不降低镇痛效力。谷氨酸8的取代可能是设计β-内啡肽拮抗剂的更可靠方法之一。
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