中国药物化学杂志
中國藥物化學雜誌
중국약물화학잡지
Chinese Journal of Medicinal Chemistry
2001年
1期
32-36
,共5页
HCMV蛋白酶%拟肽类抑制剂%设计%组合构建块%异腈前体%合成
HCMV蛋白酶%擬肽類抑製劑%設計%組閤構建塊%異腈前體%閤成
HCMV단백매%의태류억제제%설계%조합구건괴%이정전체%합성
根据HCMV蛋白酶晶体结构和拟肽类抑制剂与酶复合物的晶体结构数据,设计了拟肽类HCMV蛋白酶抑制剂化合物库Ⅰ,并拟采取液相组合方式,通过两步策略,首先由四种构建块分子:羧酸、胺、醛或酮和异腈,经Ugi四组分缩合反应生成Ⅱ,然后氧化来合成化学库。介绍其中最重要的构建块异腈Ⅲ的前体Ⅳ的合成。首先将酒石酸二乙酯由相应胺进行酰胺化产生酒石酸二酰胺Ⅴ。酒石酸二酰胺用过碘酸氧化裂解产生乙醛酸酰胺Ⅵ,然后不经分离,直接在KF-氧化铝的催化下完成硝基乙烷的加成。由此生成的2-羟基-3-硝基丁酰胺Ⅶ可经Zn+NH4Cl或Zn+NH4Cl+催化量10%Pd-C还原为2-羟基-3-氨基丁酰胺Ⅷ,再经过氨基的甲酰化生成2-羟基-3-甲酰胺基丁酰胺Ⅳ。但是在甲酸乙酯存在下,用H2/Pd-C对Ⅶ的硝基进行还原,得到的Ⅷ中的氨基可当即被甲酰化,使由Ⅶ到Ⅳ的两步反应一步完成。
根據HCMV蛋白酶晶體結構和擬肽類抑製劑與酶複閤物的晶體結構數據,設計瞭擬肽類HCMV蛋白酶抑製劑化閤物庫Ⅰ,併擬採取液相組閤方式,通過兩步策略,首先由四種構建塊分子:羧痠、胺、醛或酮和異腈,經Ugi四組分縮閤反應生成Ⅱ,然後氧化來閤成化學庫。介紹其中最重要的構建塊異腈Ⅲ的前體Ⅳ的閤成。首先將酒石痠二乙酯由相應胺進行酰胺化產生酒石痠二酰胺Ⅴ。酒石痠二酰胺用過碘痠氧化裂解產生乙醛痠酰胺Ⅵ,然後不經分離,直接在KF-氧化鋁的催化下完成硝基乙烷的加成。由此生成的2-羥基-3-硝基丁酰胺Ⅶ可經Zn+NH4Cl或Zn+NH4Cl+催化量10%Pd-C還原為2-羥基-3-氨基丁酰胺Ⅷ,再經過氨基的甲酰化生成2-羥基-3-甲酰胺基丁酰胺Ⅳ。但是在甲痠乙酯存在下,用H2/Pd-C對Ⅶ的硝基進行還原,得到的Ⅷ中的氨基可噹即被甲酰化,使由Ⅶ到Ⅳ的兩步反應一步完成。
근거HCMV단백매정체결구화의태류억제제여매복합물적정체결구수거,설계료의태류HCMV단백매억제제화합물고Ⅰ,병의채취액상조합방식,통과량보책략,수선유사충구건괴분자:최산、알、철혹동화이정,경Ugi사조분축합반응생성Ⅱ,연후양화래합성화학고。개소기중최중요적구건괴이정Ⅲ적전체Ⅳ적합성。수선장주석산이을지유상응알진행선알화산생주석산이선알Ⅴ。주석산이선알용과전산양화렬해산생을철산선알Ⅵ,연후불경분리,직접재KF-양화려적최화하완성초기을완적가성。유차생성적2-간기-3-초기정선알Ⅶ가경Zn+NH4Cl혹Zn+NH4Cl+최화량10%Pd-C환원위2-간기-3-안기정선알Ⅷ,재경과안기적갑선화생성2-간기-3-갑선알기정선알Ⅳ。단시재갑산을지존재하,용H2/Pd-C대Ⅶ적초기진행환원,득도적Ⅷ중적안기가당즉피갑선화,사유Ⅶ도Ⅳ적량보반응일보완성。
The human cytomegalovirus(HCMV)is a member of the herpesvirusfamily infecting 40%~80% of the general population.HCMV can cause fatal infections in immunocompromised individuals.HCMV encodes a serine protease that is essential for viral replication and is a potential target for antiviral drug development.In this paper a peptidomimetic library Ⅰ for HCMV protease inhibitor was designed based on the interactions between the protease active site and its peptidomimetic inhibitors.The library was synthesized in the manner of liquid-phase combinatorial synthesis,by a two-step strategy.Firstly by the Ugi four-component condensation reaction,from four kinds of building blocks-carboxylic acids,amines,aldehydes or ketones and isocyanides,then followed by oxidation of the product Ⅱ to form the library.The isocyanide Ⅲ was the most important block for building up the library.The syntheses of the former compounds Ⅳ of the isocyanides were described.Tartaric acid diamides Ⅴ were obtained first from diethyl tartrate in good yield.The oxidative scission of Ⅴ by periodic acid gave glycoxylic amides Ⅵ,which were then nitroethylated immediately without working up and produce 2-hydroxy-3-nitrobutyric amide Ⅶ catalyzed by KF-alumina.The nitro group of Ⅶ was then reduced by Zn+NH4Cl or Zn+NH4Cl+catalytic amount of 10%Pd-C to yield 2-hydroxy-3-aminobutyric amide Ⅶ,and followed by formylation of the amino group to give 2-hydroxy-3-formamidobutyric amide Ⅴ.With the occurrence of H2/Pd-C and ethyl formic ester,the reduction of the nitro group and the formylation of the amino group could be finished in one step.By this way three isocyanide formers were synthesized with the R group benzyl,cyclohexyl and 2-cyclohexenylethyl respectively.
