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针对血红素鉴定细胞毒性剂。

Targeting heme for the identification of cytotoxic agents.

机构信息

Geisinger Clinic, Danville, PA 17822, USA.

出版信息

Anticancer Agents Med Chem. 2013 Mar;13(3):515-22.

Abstract

Certain tumor types have an increased capacity for heme synthesis, which serves as the basis for photodynamic therapy. Heme also serves as the target for the anti-malaria drug artemisinin, which has also been used as an anti-cancer drug. We developed a high-throughput screening assay to identify heme interacting (HI) compounds, which included imidazole, pyridine, carbonitrile, isocyanide, and quinoline core structures that are known to interact with heme or hemin. The cytotoxicity of several of the compounds towards human leukemia cell lines could be modulated by increasing or decreasing heme synthesis. Spectral analysis indicated that distinct molecular interactions occurred with heme, suggesting that HI compounds appear to target heme with exquisite specificity. These studies suggest that heme may serve as a novel therapeutic target for cancer drug discovery.

摘要

某些肿瘤类型具有增加血红素合成的能力,这是光动力疗法的基础。血红素也是抗疟药物青蒿素的靶标,青蒿素也被用作抗癌药物。我们开发了一种高通量筛选测定法来鉴定血红素相互作用(HI)化合物,其中包括咪唑、吡啶、腈、异氰化物和喹啉核心结构,已知这些结构与血红素或血红素结合。几种化合物对人白血病细胞系的细胞毒性可以通过增加或减少血红素合成来调节。光谱分析表明,血红素发生了不同的分子相互作用,这表明 HI 化合物似乎以极高的特异性靶向血红素。这些研究表明,血红素可能成为癌症药物发现的新的治疗靶点。

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