一种通过十八烷基甘油残基连接齐多夫定（AZT）和膦甲酸钠（PFA）的新型抗病毒双链药物的合成及其体外活性

Synthesis and in vitro activities of a new antiviral duplex drug linking Zidovudine (AZT) and Foscarnet (PFA) via an octadecylglycerol residue.

作者信息

Schott Herbert, Hamprecht Klaus, Schott Sarah, Schott Timm C, Schwendener Reto A

机构信息

Institute for Organic Chemistry, University Tuebingen, Auf der Morgenstelle 18, D-72076 Tuebingen, Germany.

出版信息

Bioorg Med Chem. 2009 Jan 1;17(1):303-10. doi: 10.1016/j.bmc.2008.10.081. Epub 2008 Nov 5.

DOI:10.1016/j.bmc.2008.10.081

PMID:19010684

Abstract

To prepare a new antiviral duplex drug linking Zidovudine (AZT) and Foscarnet (PFA) via a lipophilic octadecylglycerol residue we condensed 1-O-4-monomethoxytrityl-3-O-octadecyl-sn-glycerol-2-hydrogenphosphonate obtained from 3-O-octadecyl-sn-glycerol with AZT by the phosphonate method. The purified condensation product was de-tritylated resulting in 3'-azido-3'-deoxythymidylyl-(5'-->2-O)-3-O-octadecyl-sn-glycerol, followed by treatment with (ethoxycarbonyl)phosphoric dichloride. The resulting 3'-azido-3'-deoxy-thymidylyl-(5'-->2)-3-O-octadecyl-sn-glycerol-1-O-(ethoxycarbonyl)phosphonate was purified by preparative RP-18 column chromatography. The antiviral duplex drug 3'-azido-3'-deoxythymidylyl-(5'-->2-O)-3-O-octadecyl-sn-glycerol-1-O-phosphonoformate trisodium salt (AZT-lipid-PFA) was obtained after alkaline cleavage of the phosphonoformate ethylester residue. The overall yield of the five step synthesis performed at gram scale was about 30%. According to a supposed pathway AZT-lipid-PFA could be cleaved to yield a mixture of different antiviral compounds such as AZT, AZT-5'-monophosphate, octadecylglycerol-AZT, PFA and octadecylglycerol-PFA, possibly producing additive and/or synergistic antiviral effects. In vitro studies showed that the duplex drug exhibits antiviral activities against HIV and especially against drug-resistant strains and clinical isolates of HSV and HCMV. The E(50) values of AZT-lipid-PFA against HIV ranged between 170 and 200 nM. The half-maximal inhibitory doses (IC(50)) against highly acyclovir (ACV)-resistant HSV isolates determined by a plaque reduction assay ranged between 1.87 and 4.59 microM. Using ganciclovir (GCV)-sensitive, GCV resistant and drug cross-resistant HCMV strains the IC(50)-values of AZT-lipid-PFA were between 2.78 and 1.18 microM. With regard to PFA, the IC(50)-value of AZT-lipid-PFA determined on a multi-drug-resistant HCMV strain was about 90-fold lower than that of PFA, demonstrating the superior antiviral effect of the duplex-drug.

摘要

为了制备一种通过亲脂性十八烷基甘油残基连接齐多夫定（AZT）和膦甲酸（PFA）的新型抗病毒双链体药物，我们采用膦酸酯法将由3 - O - 十八烷基 - sn - 甘油制得的1 - O - 4 - 单甲氧基三苯甲基 - 3 - O - 十八烷基 - sn - 甘油 - 2 - 氢膦酸酯与AZT缩合。纯化后的缩合产物进行脱三苯甲基反应，得到3'-叠氮基 - 3'-脱氧胸苷酰基 - (5'→2 - O) - 3 - O - 十八烷基 - sn - 甘油，随后用二氯（乙氧羰基）磷酸酯处理。所得的3'-叠氮基 - 3'-脱氧 - 胸苷酰基 - (5'→2) - 3 - O - 十八烷基 - sn - 甘油 - 1 - O - （乙氧羰基）膦酸酯通过制备型RP - 18柱色谱法纯化。在膦甲酸乙酯残基进行碱性裂解后，得到抗病毒双链体药物3'-叠氮基 - 3'-脱氧胸苷酰基 - (5'→2 - O) - 3 - O - 十八烷基 - sn - 甘油 - 1 - O - 膦甲酸三钠盐（AZT - 脂质 - PFA）。以克级规模进行的五步合成的总产率约为30%。根据推测的途径，AZT - 脂质 - PFA可能被裂解，产生不同抗病毒化合物的混合物，如AZT、AZT - 5'-单磷酸、十八烷基甘油 - AZT、PFA和十八烷基甘油 - PFA，可能产生相加和/或协同的抗病毒作用。体外研究表明，该双链体药物对HIV具有抗病毒活性，尤其对耐药菌株以及HSV和HCMV的临床分离株有活性。AZT - 脂质 - PFA对HIV的E(50)值在170至200 nM之间。通过蚀斑减少试验测定，其对高阿昔洛韦（ACV）耐药的HSV分离株的半数最大抑制剂量（IC(50)）在1.87至4.59 microM之间。使用更昔洛韦（GCV）敏感、GCV耐药和药物交叉耐药的HCMV菌株，AZT - 脂质 - PFA的IC(50)值在2.78至1.18 microM之间。关于PFA，在一种多药耐药的HCMV菌株上测定的AZT - 脂质 - PFA的IC(50)值比PFA低约90倍，证明了该双链体药物具有更强的抗病毒效果。