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Evaluation of Polyamine Transport Inhibitors in a Drosophila Epithelial Model Suggests the Existence of Multiple Transport Systems

机译:果蝇上皮模型中的多胺运输抑制剂的评估表明存在多种运输系统。

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摘要

Increased polyamine biosynthesis activity and an active polyamine transport system are characteristics of many cancer cell lines and polyamine depletion has been shown to be a viable anticancer strategy. Polyamine levels can be depleted by difluoromethylornithine (DFMO), an inhibitor of the key polyamine biosynthesis enzyme ornithine decarboxylase (ODC). However, malignant cells frequently circumvent DFMO therapy by up-regulating polyamine import. Therefore, there is a need to develop compounds that inhibit polyamine transport. Collectively, DFMO and a polyamine transport inhibitor (PTI) provide the basis for a combination therapy leading to effective intracellular polyamine depletion. We have previously shown that the pattern of uptake of a series of polyamine analogues in a Drosophila model epithelium shares many characteristics with mammalian cells, indicating a high degree of similarity between the mammalian and Drosophila polyamine transport systems. In this report, we focused on the utility of the Drosophila epithelial model to identify and characterize polyamine transport inhibitors. We show that a previously identified inhibitor of transport in mammalian cells has a similar activity profile in Drosophila. The Drosophila model was also used to evaluate two additional transport inhibitors. We further demonstrate that a cocktail of polyamine transport inhibitors is more effective than individual inhibitors, suggesting the existence of multiple transport systems in Drosophila. Our findings reinforce the similarity between the Drosophila and mammalian transport systems and the value of the Drosophila model to provide inexpensive early screening of molecules targeting the transport system.
机译:增加的多胺生物合成活性和活跃的多胺转运系统是许多癌细胞系的特征,而多胺的消耗已被证明是一种可行的抗癌策略。多胺水平可以通过二氟甲基鸟氨酸(DFMO)消耗,二氟甲基鸟氨酸是关键的多胺生物合成酶鸟氨酸脱羧酶(ODC)的抑制剂。但是,恶性细胞通常会通过上调多胺的导入来规避DFMO治疗。因此,需要开发抑制多胺转运的化合物。 DFMO和多胺转运抑制剂(PTI)共同为导致有效的细胞内多胺耗竭的联合疗法提供了基础。我们以前已经表明,果蝇模型上皮细胞摄取一系列多胺类似物的模式与哺乳动物细胞具有许多特征,这表明哺乳动物和果蝇多胺转运系统之间具有高度相似性。在本报告中,我们集中于果蝇上皮模型在鉴定和表征多胺转运抑制剂方面的实用性。我们表明,先前确定的哺乳动物细胞运输抑制剂在果蝇中具有相似的活性。果蝇模型也用于评估另外两种转运抑制剂。我们进一步证明,多胺转运抑制剂的混合物比单独的抑制剂更有效,这表明果蝇中存在多种转运系统。我们的发现加强了果蝇和哺乳动物运输系统之间的相似性,并增强了果蝇模型的价值,以提供廉价,早期筛选靶向运输系统的分子的价值。

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