抑制细胞迁移并靶向半乳糖凝集素-3碳水化合物结合位点之外区域的四氢异喹啉天然产物类似物。
Analogs of tetrahydroisoquinoline natural products that inhibit cell migration and target galectin-3 outside of its carbohydrate-binding site.
作者信息
Kahsai Alem W, Cui Junru, Kaniskan H Umit, Garner Philip P, Fenteany Gabriel
机构信息
Department of Chemistry, University of Connecticut, Storrs, Connecticut 06269, USA.
出版信息
J Biol Chem. 2008 Sep 5;283(36):24534-45. doi: 10.1074/jbc.M800006200. Epub 2008 Jun 13.
Cell migration is central to a number of normal and disease processes. Small organic molecules that inhibit cell migration have potential as both research probes and therapeutic agents. We have identified two tetrahydroisoquinoline natural product analogs with antimigratory activities on Madin-Darby canine kidney epithelial cells: a semisynthetic derivative of quinocarmycin (also known as quinocarcin), DX-52-1, and a more complex synthetic molecule, HUK-921, related to the naphthyridinomycin family. It has been assumed that the cellular effects of reactive tetrahydroisoquinolines result from the alkylation of DNA. We have reported previously that the primary target of DX-52-1 relevant to cell migration appears to be the membrane-cytoskeleton linker protein radixin. Here we extend the analysis of the protein targets of DX-52-1, reporting that the multifunctional carbohydrate-binding protein galectin-3 is a secondary target of DX-52-1 that may also be relevant to the antimigratory effects of both DX-52-1 and HUK-921. All known inhibitors of galectin-3 target its beta-galactoside-binding site in the carbohydrate recognition domain. However, we found that DX-52-1 and HUK-921 bind galectin-3 outside of its beta-galactoside-binding site. Intriguingly HUK-921, although a less potent inhibitor of cell migration than DX-52-1, had far greater selectivity for galectin-3 over radixin, exhibiting little binding to radixin, both in vitro and in cells. Overexpression of galectin-3 in cells led to a dramatic increase in cell adhesion on different extracellular matrix substrata as well as changes in cell-cell adhesion and cell motility. Galectin-3-overexpressing cells had greatly reduced sensitivity to DX-52-1 and HUK-921, and these compounds caused a change in localization of the overexpressed galectin-3 and reversion of the cells to a more normal morphology. The converse manipulation, RNA interference-based silencing of galectin-3 expression, resulted in reduced cell-matrix adhesion and cell migration. In aggregate, the data suggest that DX-52-1 and HUK-921 inhibit a carbohydrate binding-independent function of galectin-3 that is involved in cell migration.
细胞迁移是许多正常和疾病过程的核心。抑制细胞迁移的小分子有机化合物具有作为研究探针和治疗药物的潜力。我们已经鉴定出两种对Madin-Darby犬肾上皮细胞具有抗迁移活性的四氢异喹啉天然产物类似物:醌癌素(也称为醌癌菌素)的半合成衍生物DX-52-1,以及一种与萘啶霉素家族相关的更复杂的合成分子HUK-921。人们一直认为活性四氢异喹啉的细胞效应是由DNA烷基化引起的。我们之前曾报道,与细胞迁移相关的DX-52-1的主要靶点似乎是膜-细胞骨架连接蛋白根蛋白。在此,我们扩展了对DX-52-1蛋白质靶点的分析,报告多功能碳水化合物结合蛋白半乳凝素-3是DX-52-1的次要靶点,它可能也与DX-52-1和HUK-921的抗迁移作用有关。所有已知的半乳凝素-3抑制剂都靶向其碳水化合物识别结构域中的β-半乳糖苷结合位点。然而,我们发现DX-52-1和HUK-921在半乳凝素-3的β-半乳糖苷结合位点之外与其结合。有趣的是,HUK-921虽然作为细胞迁移抑制剂的效力不如DX-52-1,但对半乳凝素-3的选择性远高于根蛋白,在体外和细胞内与根蛋白的结合都很少。细胞中半乳凝素-3的过表达导致细胞在不同细胞外基质底物上的黏附显著增加,以及细胞间黏附和细胞运动性的改变。过表达半乳凝素-3的细胞对DX-52-1和HUK-921的敏感性大大降低,这些化合物导致过表达的半乳凝素-3的定位发生变化,并使细胞恢复到更正常的形态。相反的操作,即基于RNA干扰的半乳凝素-3表达沉默,导致细胞-基质黏附和细胞迁移减少。总体而言,这些数据表明DX-52-1和HUK-921抑制了半乳凝素-3参与细胞迁移的不依赖碳水化合物结合的功能。
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