Drug Design and Synthesis Section, Chemical Biology Research Branch, NIDA and NIAAA, National Institutes of Health, Department of Health and Human Services, 5625 Fishers Lane, Room 4N03, Bethesda, Maryland 20892-9415, USA.
J Nat Prod. 2012 Apr 27;75(4):661-8. doi: 10.1021/np2008957. Epub 2012 Feb 23.
20R,21R-Epoxyresibufogenin-3-formate (1) and 20S,21S-epoxyresibufogenin-3-formate (2) were synthesized from commercial resibufogenin (3) using known procedures. The major product (1) was dextrorotatory, as was the major product from the reported synthesis of epoxyresibufogenin-3-formate; however, the literature (+)-compound was assigned the 20S,21S-configuration on the basis of NMR data. We have now unequivocally determined, using single-crystal X-ray structure analyses of the major and minor products of the synthesis and of their derivatives, that the major product from the synthesis was (+)-20R,21R-epoxyresibufogenin-3-formate (1). Our minor synthetic product was determined to have the (-)-20S,21S-configuration (2). The (+)-20R,21R-compound 1 has been found to have high affinity for the IL-6 receptor and to act as an IL-6 antagonist. A greatly improved synthesis of 1 was achieved through oxidation of preformed resibufogenin-3-formate. This has enabled us to prepare, from the very expensive commercial resibufogenin, considerably larger quantities of 1, the only known nonpeptide small-molecule IL-6 antagonist.
20R,21R-环氧响尾蛇毒素-3-甲酸盐(1)和 20S,21S-环氧响尾蛇毒素-3-甲酸盐(2)是由商业响尾蛇毒素(3)经已知步骤合成的。主要产物(1)为右旋,与环氧响尾蛇毒素-3-甲酸盐的报道合成中的主要产物相同;然而,文献中的(+)-化合物是根据 NMR 数据分配 20S,21S-构型的。我们现在已经通过对合成的主要和次要产物及其衍生物的单晶 X 射线结构分析,明确确定了主要产物是(+)-20R,21R-环氧响尾蛇毒素-3-甲酸盐(1)。我们的次要合成产物被确定为(-)-20S,21S-构型(2)。(+)-20R,21R-化合物 1 已被发现对 IL-6 受体具有高亲和力,并作为 IL-6 拮抗剂。通过预形成的响尾蛇毒素-3-甲酸盐的氧化,实现了 1 的大大改进的合成。这使我们能够从非常昂贵的商业响尾蛇毒素中制备出大量的 1,1 是唯一已知的非肽小分子 IL-6 拮抗剂。
