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Organoselenium Compounds as Novel Adjuvants of Chemotherapy Drugs—A Promising Approach to Fight Cancer Drug Resistance

机译:有机烯化合物作为化疗药物的新佐剂 - 一种有希望的抗癌耐药性的方法

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摘要

Malignant diseases present a serious public health burden and their treatment with traditional chemotherapy cannot be considered an all-round solution, due to toxic side effects. Selenium compounds (Se-compounds) have received substantial attention in medicinal chemistry, especially in experimental chemotherapy, both as cytotoxic agents and adjuvants in chemotherapy. A checkerboard microplate method was applied to study the drug interactions of Se-compounds and clinically relevant chemotherapeutic drugs against the multidrug-resistant (MDR) subtype of mouse t-lymphoma cells overexpressing the ABCB1 transporter. Se-compounds showed synergistic interactions with chemotherapeutic agents targeting the topoisomerase enzymes or the microtubule apparatus. The ketone-containing selenoesters showed synergism at lower concentrations (1.25 µM). Most of the tested compounds interacted antagonistically with alkylating agents and verapamil. A thiophene-containing Se-compound showed synergism with all tested drugs, except cisplatin. While the exact mechanism of drug interactions is yet unknown, the potency of the selenocompounds as efflux pump inhibitors or the potentiation of their efficacy as reactive oxygen species modulators may play a role in their complementary activity against the tested MDR lymphoma cell line.
机译:恶性疾病提出了严重的公共卫生负担,并且由于毒性副作用,他们的传统化疗的治疗不能被视为全圆的解决方案。硒化合物(Se-化合物)在药物化学中获得了大量关注,特别是在实验化疗,既是化学疗法中的细胞毒性剂和佐剂。应用棋盘噬藻体方法研究Se-化合物和临床相关化疗药物对多药物抗性(MDR)亚型过表达ABCB1转运蛋白的多药物抗性(MDR)亚型的药物相互作用。 Se-化合物显示出与靶向拓扑异构酶或微管装置的化学治疗剂的协同相互作用。含酮的SelenoSters在较低浓度(1.25μm)下表现出协同作用。大多数测试化合物用烷基化试剂和维拉帕米相互作用。除了顺铂之外,含含噻吩的Se-化合物显示出与所有测试药物的协同作用。虽然药物相互作用的确切机制尚不清楚,但Selenocompounds作为流动泵抑制剂的效力或它们作为反应性氧物质调节剂的功效的增强可能在对测试的MDR淋巴瘤细胞系中的互补活动中起作用。

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