Six highly active mu-selective opioid peptides identified from two synthetic combinatorial libraries.

Peptide research Pub Date : 1995-05-01
C T Dooley, R A Kaplan, N N Chung, P W Schiller, J M Bidlack, R A Houghten
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Abstract

Two synthetic combinatorial libraries (SCLs) were prepared, each composed of 52,128,400 L-amino acid hexapeptides, one with and the other without an N-terminal acetyl moiety. The two libraries were used in conjunction with an iterative selection process to identify individual peptides capable of inhibiting the binding of the mu-selective opioid peptide [3H]-[D-Ala2,MePhe4,Gly-ol5]enkephalin to rat brain homogenates. As reported previously, when using the nonacetylated SCL the first five residues identified corresponded exactly to methionine- and leucine-enkephalin, both of which are endogenous opioid peptides. The iterative identification process has now been completed for two additional mixtures found to have activity in the initial screening of this SCL. Two new series unrelated to the enkephalins have been identified: YPFGFO-NH2 and WWPKHO-NH2 (where O = one of the 20 L-amino acids). Individual peptides from each of these were found to be agonists at the mu receptor and have high affinity (IC50 values of the most active peptides were 10-15 nM) and selectivity for the mu receptor. In addition to the acetalins (described previously), two new series have now been identified from the acetylated library: Ac-FRWWYO-NH2 and Ac-RWIG-WO-NH2 (IC50 values of the most active peptides were 5-30 nM). Ac-FRWWYM-NH2 was determined to be an agonist at the mu receptor, whereas Ac-RWIGWR-NH2 was found to be an antagonist at this receptor.

从两个合成组合文库中鉴定出六个高活性的多选择性阿片肽。
制备了两个合成组合文库(SCLs),每个文库由52,128,400个l -氨基酸六肽组成,其中一个含有n端乙酰基片段,另一个不含n端乙酰基片段。将这两个文库与迭代选择过程结合使用,以鉴定能够抑制微选择性阿片肽[3H]-[D-Ala2,MePhe4,Gly-ol5]脑啡肽与大鼠脑浆液结合的单个肽。如前所述,当使用非乙酰化的SCL时,鉴定出的前五个残基完全对应于蛋氨酸-和亮氨酸-脑啡肽,两者都是内源性阿片肽。在该SCL的初步筛选中发现了另外两种具有活性的混合物,现在已经完成了迭代鉴定过程。已经发现了两个与脑啡肽无关的新系列:YPFGFO-NH2和WWPKHO-NH2(其中O = 20个l -氨基酸之一)。研究发现,这些肽中的每一个都是mu受体的激动剂,并且对mu受体具有高亲和力(最活跃肽的IC50值为10-15 nM)和选择性。除了前面描述的乙酰化肽外,现在还从乙酰化文库中鉴定出两个新的系列:Ac-FRWWYO-NH2和Ac-RWIG-WO-NH2(最活性肽的IC50值为5-30 nM)。Ac-FRWWYM-NH2被确定为mu受体的激动剂,而Ac-RWIGWR-NH2被发现是该受体的拮抗剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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