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ATN-224 的氧化还原相关抗黑色素瘤活性。

Redox-related antimelanoma activity of ATN-224.

机构信息

Clinical Pharmacology and Developmental Therapeutics, University of California Irvine Chao Family Comprehensive Cancer Center, Orange, California, USA.

出版信息

Melanoma Res. 2009 Dec;19(6):350-60. doi: 10.1097/CMR.0b013e32832c6324.

Abstract

Melanoma cells characteristically produce increased levels of reactive oxygen species (ROS) because of the metal-binding properties of melanin and loss of structural integrity of the melanosome. Agents that deplete gluthathione or inhibit superoxide dismutase, thereby blocking ROS scavenging mechanisms, may be selectively toxic to melanoma. To determine whether the inhibition of ROS scavenging could potentiate alkylator activity, we evaluated the activity of tetrathiomolybdate (ATN-224), a superoxide dismutase inhibitor, alone and in combination with temozolomide, on five melanoma cell lines. We also determined whether the ATN-224 would act synergistically with other agents that interfere with ROS scavenging. We found that the combination of ATN-224 and temozolomide generally exhibited additive cytotoxic effects on the cell lines tested. ATN-224 acted synergistically with buthionine sulfoximine, an agent that causes gluthathione depletion. Combinations of ATN-224 with arsenic trioxide, which may deplete glutathione, or disulfiram, an agent that interferes with recycling of glutathione, were antagonistic. These data suggest that strategically tailoring combination regimens that include ATN-224 and target ROS may be a viable approach to advance the treatment of melanoma.

摘要

黑色素瘤细胞由于黑色素的金属结合特性和黑素小体结构完整性的丧失,通常会产生高水平的活性氧物种 (ROS)。耗尽谷胱甘肽或抑制超氧化物歧化酶的药物,从而阻断 ROS 清除机制,可能对黑色素瘤具有选择性毒性。为了确定抑制 ROS 清除是否可以增强烷化剂的活性,我们单独评估了超氧化物歧化酶抑制剂四硫钼酸盐 (ATN-224) 以及与替莫唑胺联合应用于五种黑色素瘤细胞系的活性。我们还确定了 ATN-224 是否会与其他干扰 ROS 清除的药物协同作用。我们发现,在测试的细胞系中,ATN-224 与替莫唑胺联合使用通常表现出相加的细胞毒性作用。ATN-224 与导致谷胱甘肽耗竭的药物丁硫氨酸亚砜胺协同作用。ATN-224 与三氧化二砷(可能耗尽谷胱甘肽)或干扰谷胱甘肽循环的药物双硫仑的组合是拮抗的。这些数据表明,有策略地调整包括 ATN-224 和靶向 ROS 的联合治疗方案可能是推进黑色素瘤治疗的可行方法。

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