Department of Pharmacy, Faculty of Health Sciences, UiT The Arctic University of Norway, Breivika, NO-9037 Tromsø, Norway.
Org Biomol Chem. 2013 Dec 21;11(47):8202-8. doi: 10.1039/c3ob41941j. Epub 2013 Oct 23.
The cyclopentapeptide CXCR4 antagonist FC131 (cyclo(-Arg(1)-Arg(2)-2-Nal(3)-Gly(4)-D-Tyr(5)-), 2; 2-Nal = 3-(2-naphthyl)alanine) represents an excellent starting point for development of novel drug-like ligands with therapeutic potential in HIV, cancer, stem-cell mobilization, inflammation, and autoimmune diseases. While the structure-activity relationships for Arg(1), Arg(2), and Gly(4) are well established, less is understood about the roles of the aromatic residues 2-Nal(3) and D-Tyr(5). Here we report further structure-activity relationship studies of these two positions, which showed that (i) the distal aromatic ring of the 2-Nal(3) side chain is required in order to maintain high potency and (ii) replacement of D-Tyr(5) with conformationally constrained analogues results in significantly reduced activity. However, a simplified analogue that contained Gly instead of D-Tyr(5) was only 13-fold less potent than 2, which means that the D-Tyr(5) side chain is dispensable. These findings were rationalized based on molecular docking, and the collective structure-activity data for the cyclopentapeptides suggest that appropriately designed Arg(2)-2-Nal(3) dipeptidomimetics have potential as CXCR4 antagonists.
环戊肽 CXCR4 拮抗剂 FC131(环(-Arg(1)-Arg(2)-2-Nal(3)-Gly(4)-D-Tyr(5)-),2;2-Nal = 3-(2-萘基)丙氨酸)是开发具有治疗潜力的新型药物样配体的绝佳起点,可用于治疗 HIV、癌症、干细胞动员、炎症和自身免疫性疾病。虽然 Arg(1)、Arg(2)和 Gly(4)的结构-活性关系已经得到很好的建立,但对于芳香族残基 2-Nal(3)和 D-Tyr(5)的作用了解较少。在这里,我们报告了对这两个位置的进一步结构-活性关系研究,结果表明:(i)为了保持高活性,需要 2-Nal(3)侧链的远端芳香环;(ii)用构象受限的类似物替换 D-Tyr(5)会导致活性显著降低。然而,含有 Gly 而不是 D-Tyr(5)的简化类似物仅比 2 低 13 倍,这意味着 D-Tyr(5)侧链是可有可无的。这些发现基于分子对接进行了合理化,并对环戊肽的整体结构-活性数据进行了分析,表明经过适当设计的 Arg(2)-2-Nal(3)二肽模拟物有可能成为 CXCR4 拮抗剂。
