De Clercq E, Yamamoto N, Pauwels R, Balzarini J, Witvrouw M, De Vreese K, Debyser Z, Rosenwirth B, Peichl P, Datema R
Rega Institute for Medical Research, Katholieke Universiteit Leuven, Belgium.
Antimicrob Agents Chemother. 1994 Apr;38(4):668-74. doi: 10.1128/AAC.38.4.668.
Bicyclams, in which the cyclam (1,4,8,11-tetraazacyclotetradecane) moieties are tethered via an aliphatic bridge (i.e., propylene, as in JM2763) are potent and selective inhibitors of human immunodeficiency virus type 1 (HIV-1) and type 2 (HIV-2) (E. De Clercq, N. Yamamoto, R. Pauwels, M. Baba, D. Schols, H. Nakashima, J. Balzarini, Z. Debyser, B. A. Murrer, D. Schwartz, D. Thornton, G. Bridger, S. Fricker, G. Henson, M. Abrams, and D. Picker, Proc. Natl. Acad. Sci. USA 89:5286-5290, 1992). We have now found that the bicyclam JM3100, in which the cyclam moieties are tethered by an aromatic bridge [i.e., phenylenebis(methylene)], inhibits the replication of various HIV-1 and HIV-2 strains in various cell lines at a 50% effective concentration (EC50) of 1 to 10 ng/ml, which is about 100-fold lower than the concentration required for JM2763 to inhibit HIV replication and at least 100,000-fold lower than the cytotoxic concentration (> 500 micrograms/ml). In primary T4 lymphocytes or primary monocytes, JM3100 proved inhibitory to HIV-1(IIIB) and several clinical HIV-1 isolates at an EC50 of less than 1 ng/ml. On the basis of time-of-addition experiments, JM3100 appeared to interact with a viral uncoating event, and this was further corroborated by an uncoating assay in which RNase sensitivity of [5-3H]uridine-labeled virions was monitored. In addition, but possibly mechanistically related, JM3100 blocks formation of infectious particles. JM3100 was also found to interfere directly with virus-induced syncytium formation, albeit at a higher concentration (1 to 2 microgram/ml) than that required for inhibition of viral replication. Following subcutaneous injection of 10 mg of JM3100 per kg of body weight to rabbits, anti-HIV activity was detected in serum corresponding to serum drug levels exceeding for at least 6 h by >100-fold the EC(50) required to inhibit HIV replication in vitro. When combined with either 3'-azido-2',3' -dideoxythymidine or 2',3' -dideoxyinosine, JM3100 achieved a additive inhibition of HIV replication, and when repeatedly subcultivated in the presence of JM3100, the virus remained sensitive to the compound for at least 30 passages (120 days) in cell culture.
双环胺类化合物中,环胺(1,4,8,11-四氮杂环十四烷)部分通过脂肪族桥连(如在JM2763中为亚丙基)相连,是1型人类免疫缺陷病毒(HIV-1)和2型人类免疫缺陷病毒(HIV-2)的强效和选择性抑制剂(E. 德克勒克、N. 山本、R. 保韦尔斯、M. 巴巴、D. 斯科尔斯、H. 中岛、J. 巴尔扎里尼、Z. 德贝塞尔、B. A. 默勒、D. 施瓦茨、D. 桑顿、G. 布里杰、S. 弗里克、G. 亨森、M. 艾布拉姆斯和D. 皮克,《美国国家科学院院刊》89:5286 - 5290,1992年)。我们现已发现,双环胺JM3100中,环胺部分通过芳香族桥连[即亚苯基双(亚甲基)]相连,在各种细胞系中对多种HIV-1和HIV-2毒株的复制具有抑制作用,其50%有效浓度(EC50)为1至10纳克/毫升,这比JM2763抑制HIV复制所需浓度低约100倍,比细胞毒性浓度(>500微克/毫升)至少低100,000倍。在原代T4淋巴细胞或原代单核细胞中,JM3100对HIV-1(IIIB)和几种临床HIV-1分离株的EC50小于1纳克/毫升,具有抑制作用。基于添加时间实验,JM3100似乎与病毒脱壳事件相互作用,这在一项脱壳试验中得到进一步证实,该试验监测了[5-3H]尿苷标记病毒粒子的核糖核酸酶敏感性。此外,可能在机制上相关的是,JM3100可阻断感染性颗粒的形成。还发现JM3100直接干扰病毒诱导的合胞体形成,尽管其浓度(1至2微克/毫升)高于抑制病毒复制所需浓度。给兔子皮下注射每千克体重10毫克JM3100后,在血清中检测到抗HIV活性,对应血清药物水平在至少6小时内超过体外抑制HIV复制所需EC(50)的100倍以上。当与3'-叠氮-2',3'-双脱氧胸苷或2',3'-双脱氧肌苷联合使用时,JM3100对HIV复制实现了相加抑制作用,并且当在JM3100存在下反复传代培养时,病毒在细胞培养中对该化合物至少30代(120天)保持敏感。
