Wagner Carl E, Mohler Michael L, Kang Gyong Suk, Miller Duane D, Geisert Eldon E, Chang Yu-An, Fleischer Everly B, Shea Kenneth J
Department of Chemistry, University of California-Irvine, California 92697, USA.
J Med Chem. 2003 Jul 3;46(14):2823-33. doi: 10.1021/jm020326d.
A variety of amine complexes with 1-boraadamatane were synthesized and subsequently evaluated for an antiproliferative effect on CD81-enriched cell lines to provide evidence for binding and activation of CD81. CD81 is a member of the tetraspanin family of membrane proteins found in all cell lineages in the liver. CD81 signals for antiproliferation when bound by antibodies. It is known that the HCV-E2 envelope glycoprotein binds to the CD81 protein. While it is unclear whether virus entry into host cells is directly linked to virus attachment via CD81 for HCV, this step in the viral life cycle has recently proven to be an effective point of attack for other viruses including HIV and rhinoviruses. The aim of the current study concerns the synthesis of amantidine analogues by appending primary amines to 1-boraadamantane to evaluate such compounds for CD81-dependent antiproliferation of CD81-enriched cell lines (astrocyte) vs CD81-deficient cell lines (C6 glioma). If the antiproliferative effect of these amantidine analogues proves to be an effect of binding and activating CD81, then these compounds may have the potential to prevent or treat HCV infections. Each compound's potential for preventive and therapeutic activity stems from the compound's potential to block viral attachment, virus-cell fusion, or virus entry into host cells or to counter potential mechanisms of HCV immune evasion. Out of a library of over 500 compounds, including randomly selected small molecules and rationally designed small molecules, only the 1-boraadamantaneamine compounds and structurally similar analogues display a significant antiproliferative effect on the CD81-enriched astrocytes relative to the CD81-deficient cell lines. In fact, 1-boraadamantane.l-phenylalanine methyl ester complex (5), 1-boraadamantane.ethanolamine complex (8), and (S)-2-[(adamantane-1-carbonyl)amino]-3-phenylpropionic acid (15) show a dose-dependent, astrocyte-selective antiproliferative activity in the concentration range 0.1-10 microM. This is consistent with the binding and activation of CD81 and represents a 2-fold improvement compared to the clinically prescribed anti-HCV agent, amantidine, in the same concentration range. Consequently, the 1-boraadamantaneamine derivatives present a promising lead in the development of small molecules with potential to bind to CD81 and treat HCV infections.
合成了多种1-硼杂金刚烷的胺配合物,随后评估其对富含CD81的细胞系的抗增殖作用,以提供CD81结合和激活的证据。CD81是肝脏中所有细胞谱系中发现的四跨膜蛋白家族的成员。当与抗体结合时,CD81发出抗增殖信号。已知丙型肝炎病毒E2包膜糖蛋白与CD81蛋白结合。虽然尚不清楚丙型肝炎病毒进入宿主细胞是否直接通过CD81与病毒附着相关联,但病毒生命周期中的这一步骤最近已被证明是包括HIV和鼻病毒在内的其他病毒的有效攻击点。本研究的目的是通过将伯胺连接到1-硼杂金刚烷上来合成金刚烷胺类似物,以评估这些化合物对富含CD81的细胞系(星形胶质细胞)与缺乏CD81的细胞系(C6胶质瘤)的CD81依赖性抗增殖作用。如果这些金刚烷胺类似物的抗增殖作用被证明是结合和激活CD81的结果,那么这些化合物可能具有预防或治疗丙型肝炎病毒感染的潜力。每种化合物的预防和治疗活性潜力源于该化合物阻断病毒附着、病毒-细胞融合或病毒进入宿主细胞的潜力,或对抗丙型肝炎病毒免疫逃逸的潜在机制。在包含随机选择的小分子和合理设计的小分子的500多种化合物库中,只有1-硼杂金刚烷胺化合物及其结构相似的类似物相对于缺乏CD81的细胞系对富含CD81的星形胶质细胞显示出显著的抗增殖作用。事实上,1-硼杂金刚烷·L-苯丙氨酸甲酯配合物(5)、1-硼杂金刚烷·乙醇胺配合物(8)和(S)-2-[(金刚烷-1-羰基)氨基]-3-苯丙酸(15)在0.1-10微摩尔浓度范围内表现出剂量依赖性的星形胶质细胞选择性抗增殖活性。这与CD81的结合和激活一致,并且在相同浓度范围内与临床处方的抗丙型肝炎病毒药物金刚烷胺相比有2倍的改善。因此,1-硼杂金刚烷胺衍生物在开发具有与CD81结合并治疗丙型肝炎病毒感染潜力的小分子方面呈现出有前景的线索。
