Department of Medicinal Chemistry, Virginia Commonwealth University, 800 E Leigh Street, Richmond, VA 23298-0540, USA.
Eur J Med Chem. 2012 Sep;55:395-408. doi: 10.1016/j.ejmech.2012.07.049. Epub 2012 Aug 7.
Recent studies have indicated that the CCR5 chemokine receptor may be a potential target for treating prostate cancer. Thus, development of CCR5 antagonists may provide novel prostate cancer therapy. Anibamine, a novel pyridine quaternary alkaloid isolated from Aniba sp., was found to effectively compete with (125)I-gp120 in binding to the chemokine receptor CCR5, with an IC(50) = 1 μM. Anibamine is the first natural product reported as a CCR5 antagonist, and thus provides a novel structural skeleton unique from other lead compounds that have generally been identified from high-throughput screening efforts. In order to refine the lead compound's structure and improve the therapeutic index of anibamine derivatives as potential anti prostate cancer agents, the approach of "deconstruction-reconstruction-elaboration" was applied in the structure-activity relationship studies of this work. Here, we report the design, syntheses and anti prostate cancer activities of anibamine and 17 analogues. The results from the in vitro and in vivo studies described here show that this class of compounds has potential to provide novel leads as anti prostate cancer agents.
最近的研究表明,趋化因子受体 CCR5 可能是治疗前列腺癌的潜在靶点。因此,开发 CCR5 拮抗剂可能为前列腺癌治疗提供新方法。从 Aniba 属植物中分离得到的新型吡啶季铵生物碱 Anibamine 被发现能有效与(125)I-gp120 竞争结合趋化因子受体 CCR5,IC50 为 1 μM。Anibamine 是首个被报道为 CCR5 拮抗剂的天然产物,为一般通过高通量筛选得到的先导化合物提供了一个独特的新型结构骨架。为了改进先导化合物的结构并提高作为潜在抗前列腺癌药物的 Anibamine 衍生物的治疗指数,本研究采用“解构-重构-详述”方法进行了构效关系研究。在此,我们报告了 Anibamine 及其 17 种类似物的设计、合成和抗前列腺癌活性。本文所述的体外和体内研究结果表明,该类化合物具有作为抗前列腺癌药物的新型先导化合物的潜力。
