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首页> 外文期刊>Toxicology Letters: An International Journal Providing a Forum for Original and Pertinent Contributions in Toxicology Research >Aclarubicin, an anthracycline anti-cancer drug, fluorescently contrasts mitochondria and reduces the oxygen consumption rate in living human cells
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Aclarubicin, an anthracycline anti-cancer drug, fluorescently contrasts mitochondria and reduces the oxygen consumption rate in living human cells

机译:Aclarubicin,一种蒽环类抗癌药物,荧光造影线粒体并降低活性人体细胞中的氧气消耗率

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摘要

Aclarubicin (Acla), an effective anthracycline chemotherapeutic agent for hematologic cancers and solid tumors, is documented to perturb chromatin function via histone eviction and DNA topoisomerase inhibition in the nucleus, but much less attention has been paid to cytotoxic function in the cytoplasm. Here, we showed that Acla emitted fluorescence and that human cervical cancer HeLa cells exposed to Acla exhibited bright fluorescence signals in the cytoplasm when fluorescence microscopy was performed using the red filter (excitation 530-550 nm/emission 575 nm). Intriguingly, most of the signals appeared to be partitioned and enriched in entangled tubule-like structures; moreover, these signals merged with the mitochondria-specific MitoTracker signals. Notably, analysis of mitochondrial respiratory activity revealed that the oxygen consumption rate was decreased in Acla-treated cells. These findings suggest that Acla accumulates efficiently in the mitochondria of living human cells and leads to mitochondrial dysfunction, implying a previously overlooked cytotoxicity of Acla in the cytoplasm and adding mechanistic insight of the anti-cancer activity, as well as the side effects, of Acla/anthracycline-based chemotherapy.
机译:Aclarubicin(ACLA)是一种用于血液学癌和实体瘤的有效蒽环类化学治疗剂,被记录在细胞核中通过组蛋白驱逐和DNA拓扑异构酶抑制记录到Perurbol染色质功能,但在细胞质中的细胞毒性功能较小。在这里,我们表明ACLA发出的荧光,并且当使用红色过滤器进行荧光显微镜(激发530-550nm /发射575nm)时,暴露于ACLA的人宫颈癌Hela细胞在细胞质中表现出明亮的荧光信号。有趣的是,大多数信号似乎被隔开并富含缠绕的管状结构;此外,这些信号与线粒体特异性Mitotracker信号合并。值得注意的是,分析线粒体呼吸系统的分析表明,ACLA处理的细胞中氧消耗率降低。这些研究结果表明,ACLA在活性人体细胞的线粒体中有效累积,并导致线粒体功能障碍,暗示在细胞质中的ACLA的先前被忽略的细胞毒性,并加入了抗癌活动的机械洞察力,以及ACLA的副作用/蒽环类化疗。

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