Gunasekera Sarath P, Longley Ross E, Isbrucker Richard A
Division of Biomedical Marine Research, Harbor Branch Oceanographic Institution, 5600 U.S. 1 North, Fort Pierce, FL 34946, USA.
J Nat Prod. 2002 Dec;65(12):1830-7. doi: 10.1021/np0203234.
A series of 12 semisynthetic discodermolide analogues, 2-13, have been prepared using natural (+)-discodermolide (1) and evaluated for in vitro cytotoxicity against cultured murine P-388 leukemia and A-549 human adenocarcinoma cells. These semisynthetic analogues showed a significant variation of cytotoxicity and confirmed the importance of the C-7 through C-19 molecular fragment for potency. Specifically, these analogues suggested the importance of the C-11 and C-17 hydroxyl groups and the C-13 double bond for the potency of discodermolide. The preparation, structure elucidation, and biological activity of these new analogues are described.
使用天然的(+)-盘状软骨素(1)制备了一系列12种半合成盘状软骨素类似物,即2-13,并评估了它们对培养的小鼠P-388白血病细胞和A-549人腺癌细胞的体外细胞毒性。这些半合成类似物的细胞毒性表现出显著差异,并证实了C-7至C-19分子片段对药效的重要性。具体而言,这些类似物表明C-11和C-17羟基以及C-13双键对盘状软骨素的药效很重要。本文描述了这些新类似物的制备、结构解析和生物活性。