Dolence E K, Dolence J M, Poulter C D
Department of Chemistry, University of Utah, 315 South 1400 East, Room 2020, Salt Lake City, Utah 84112-0850, USA.
J Comb Chem. 2000 Sep-Oct;2(5):522-36. doi: 10.1021/cc000026m.
A solid-phase method, based on Kaiser's p-benzophenone oxime resin, was developed for the synthesis of a series of N-acetyl-S-(E, E-farnesylated) Ca(1)a(2)X tetrapeptides as potential inhibitors of recombinant Ras and a-factor converting enzyme (RCE). N-Acetyl-S-(E, E-farnesyl)-L-cysteine was coupled to resin-bound a(1)a(2) dipeptide using HOBt/DCC activation in conjunction with N-BOC chemistry. The protected farnesylated tripeptide was cleaved from the resin with simultaneous addition of the X residue by treating the resin-bound farnesylated Ca(1)a(2) tripeptide with L-amino acid benzyl ester tosylates under mildly acidic conditions. The benzyl ester was saponified, and the resulting carboxylate precipitated by ether to afford a library of tetrapeptides as a mixture of diastereomers at the cysteine center. The peptides were evaluated as inhibitors of recombinant yeast RCE endoprotease (yRCE) to obtain information about the affinity of the enzyme for the a(1)a(2)X portion of the Ca(1)a(2)X moiety.
基于凯泽对苯甲酮肟树脂开发了一种固相方法,用于合成一系列N-乙酰基-S-(E,E-法尼基化)Ca(1)a(2)X四肽,作为重组Ras和α因子转化酶(RCE)的潜在抑制剂。使用1-羟基苯并三唑/二环己基碳二亚胺(HOBt/DCC)活化并结合N-BOC化学方法,将N-乙酰基-S-(E,E-法尼基)-L-半胱氨酸与树脂结合的a(1)a(2)二肽偶联。在温和酸性条件下,通过用L-氨基酸苄酯对甲苯磺酸盐处理树脂结合的法尼基化Ca(1)a(2)三肽,将受保护的法尼基化三肽从树脂上裂解下来,同时添加X残基。苄酯被皂化,所得羧酸盐通过乙醚沉淀,得到作为半胱氨酸中心非对映异构体混合物的四肽文库。对这些肽作为重组酵母RCE内切蛋白酶(yRCE)抑制剂进行评估,以获得有关该酶对Ca(1)a(2)X部分的a(1)a(2)X亲和力的信息。
