Parker Stacy-Ann J, Hough Andrea, Wright Thomas, Lax Neil, Faruk Asef, Fofie Christian K, Simcik Rebekah, Cavanaugh Jane E, Kolber Benedict J, Tidgewell Kevin J
Graduate School of Pharmaceutical Sciences, Duquesne University Pittsburgh, PA.
Department of Neuroscience, Thiel College, Greenville, PA.
bioRxiv. 2025 Jan 22:2025.01.18.633713. doi: 10.1101/2025.01.18.633713.
Marine cyanobacteria have gained momentum in recent years as a source of novel bioactive small molecules. This paper describes the structure elucidation and pharmacological evaluation of two new, veraguamide O () and veraguamide P (), and one known, veraguamide C(), analogs isolated from a cyanobacterial collection made in the Las Perlas Archipelago of Panama. We hypothesized that these compounds would be cytotoxic in cancer cell lines. The compounds were screened against HEK-293, estrogen receptor positive (MCF-7), and triple-negative breast cancer (MDA-MB-231) cells as well as against a broad panel of membrane bound receptors. The planar structures were determined based on NMR and MS data along with comparison to previously isolated veraguamide analogs. Phylogenetic analysis of the collection suggests it to be an sp., a similar species to the cyanobacterium reported to produce other veraguamides. Veraguamide O shows no cytotoxicity (greater than 100 μM) against ER positive cells (MCF-7) with 13 μM IC against MDA-MB-231 TNBC cells. Interestingly, these compounds show affinity for the sigma2/TMEM-97 receptor making them potential leads for development of non-toxic sigma 2 targeting ligands.
近年来,海洋蓝藻作为新型生物活性小分子的来源受到了更多关注。本文描述了从巴拿马珍珠群岛采集的蓝藻样本中分离出的两种新的维拉瓜胺O()和维拉瓜胺P()以及一种已知的维拉瓜胺C()类似物的结构解析和药理评价。我们推测这些化合物对癌细胞系具有细胞毒性。这些化合物针对人胚肾细胞系293(HEK - 293)、雌激素受体阳性(MCF - 7)和三阴性乳腺癌(MDA - MB - 231)细胞以及一系列膜结合受体进行了筛选。基于核磁共振(NMR)和质谱(MS)数据并与先前分离的维拉瓜胺类似物进行比较,确定了其平面结构。对该样本的系统发育分析表明它是一种 sp.,与据报道能产生其他维拉瓜胺的蓝藻是相似物种。维拉瓜胺O对雌激素受体阳性细胞(MCF - 7)无细胞毒性(大于100 μM),对三阴性乳腺癌细胞系MDA - MB - 231的半数抑制浓度(IC)为13 μM。有趣的是,这些化合物对sigma2/TMEM - 97受体具有亲和力,使其成为开发无毒sigma 2靶向配体的潜在先导化合物。
