Kim C H, Marquez V E, Broder S, Mitsuya H, Driscoll J S
J Med Chem. 1987 May;30(5):862-6. doi: 10.1021/jm00388a020.
5-Substituted 2',3'-dideoxycytidine analogues have been synthesized and evaluated in vitro for their capabilities to protect T4+ lymphocytes from the cytopathic effects of the HTLV-III/LAV (HIV) virus, the causative agent of acquired immunodeficiency syndrome (AIDS). These analogues were designed to be more lipophilic than 2',3'-dideoxycytidine (ddC) in order to enhance central nervous system penetration. Earlier reports had shown that ddC is a potent protective agent. When ddC is substituted at the 5-position with either methyl or bromo substituents, activity is completely abolished. However, when the substitution is fluoro (5-F-ddC), both activity and potency are retained. 2',3'-Dideoxy-5-azacytidine is also protective but more toxic than ddC or 5-F-ddC. In a different approach, an attempt was made to utilize ddCMP, ddTMP, and ddAMP as preformed nucleotides in order to circumvent the generally low level of phosphorylation achieved with dideoxynucleosides which function as relatively poor substrates for the cellular kinases. Only ddAMP is as active as its nucleoside precursor. Because ddAMP is not more active than ddA at low concentrations, it is possible that the active agent is ddA which is generated from ddAMP prior to cell entry.
已合成了5-取代的2',3'-二脱氧胞苷类似物,并在体外评估了它们保护T4 +淋巴细胞免受人类嗜T淋巴细胞病毒III型/淋巴腺病相关病毒(HIV)(获得性免疫缺陷综合征(AIDS)的病原体)细胞病变效应影响的能力。设计这些类似物比2',3'-二脱氧胞苷(ddC)具有更强的亲脂性,以增强其对中枢神经系统的穿透力。早期报告表明ddC是一种有效的保护剂。当ddC在5位被甲基或溴取代时,活性完全丧失。然而,当取代基为氟(5-F-ddC)时,活性和效力均得以保留。2',3'-二脱氧-5-氮杂胞苷也具有保护作用,但比ddC或5-F-ddC毒性更大。采用另一种方法,尝试将ddCMP、ddTMP和ddAMP用作预制核苷酸,以规避通常由双脱氧核苷实现的低磷酸化水平,因为双脱氧核苷作为细胞激酶的底物相对较差。只有ddAMP与其核苷前体活性相当。由于在低浓度下ddAMP并不比ddA更具活性,所以活性剂可能是在细胞进入之前由ddAMP产生的ddA。
