New quinoxaline 1, 4-di-N-oxides: anticancer and hypoxia-selective therapeutic agents.

Ismail MM; Amin KM; Noaman E; Soliman DH; Ammar YA

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New quinoxaline 1, 4-di-N-oxides: anticancer and hypoxia-selective therapeutic agents.

机译：新的喹喔啉1，4-二-N-氧化物：抗癌和缺氧选择性治疗剂。

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A new series of quinoxaline 1,4-di-N-oxides was synthesized and evaluated for antitumor and hypoxic-selective cytotoxic activities. Antitumor activity against liver carcinoma (Hepg2) and brain tumor (U251) human cell lines were evaluated, among the tested compounds, 5b and 9b exhibited potential cytotoxic effect against Hepg2 with IC50 values of 0.77 and 0.50 microg/mL respectively, whereas, all the tested compounds lack antitumor activity against U251 human cell line. Moreover, compound 4 was the most potent hypoxia selective-cytotoxin on EAC cell line; IC50 2.5 microg/mL, potency 22 microg/mL, and was approximately 5.4-times more selective cytotoxin (HCR>40) than 3-amino-2-quinoxalinecarbonitrile1,4-dioxide (standard, HCR>7.4). Compounds 8b and 9b were more selective than the standard.

机译：合成了一系列新的喹喔啉1,4-二-N-氧化物，并评估了其抗肿瘤和低氧选择性细胞毒活性。评估了针对肝癌（Hepg2）和脑肿瘤（U251）人细胞系的抗肿瘤活性，在所测试的化合物中，5b和9b对Hepg2表现出潜在的细胞毒性作用，IC50值分别为0.77和0.50 microg / mL，而所有测试的化合物缺乏针对U251人细胞系的抗肿瘤活性。此外，化合物4是EAC细胞系中最有效的缺氧选择性细胞毒素。 IC50为2.5微克/毫升，效价为22微克/毫升，比3-氨基-2-喹喔啉甲腈1,4-二氧化物（标准，HCR> 7.4）高约5.4倍（HCR> 40）。化合物8b和9b比标准品更具选择性。

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《European Journal of Medicinal Chemistry: Chimie Therapeutique》 |2010年第7期|共6页
作者
Ismail MM; Amin KM; Noaman E; Soliman DH; Ammar YA;
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正文语种 eng
中图分类医药、卫生;劳动卫生;
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1. New quinoxaline 1, 4-di-N-oxides: anticancer and hypoxia-selective therapeutic agents. [J] . Ismail MM, Amin KM, Noaman E, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2010,第7期

机译：新的喹喔啉1，4-二-N-氧化物：抗癌和缺氧选择性治疗剂。
2. New quinoxaline 1,4-di-N-oxides. Part 1: Hypoxia-selective cytotoxins and anticancer agents derived from quinoxaline 1,4-di-N-oxides. [J] . Amin KM, Ismail MM, Noaman E, Bioorganic and Medicinal Chemistry . 2006,第20期

机译：新的喹喔啉1,4-二-N-氧化物。第1部分：来自喹喔啉1,4-二-N-氧化物的缺氧选择性细胞毒素和抗癌药。
3. Synthesis of new 2-acetyl and 2-benzoyl quinoxaline 1,4-di-N-oxide derivatives as anti-Mycobacterium tuberculosis agents. [J] . Jaso A, Zarranz B, Aldana I, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2003,第9期

机译：合成新的2-乙酰基和2-苯甲酰基喹喔啉1,4-二-N-氧化物衍生物作为抗结核分枝杆菌药物。
4. Magnetically responsive hydrogels for optimizing anticancer therapeutic delivery profiles [C] . Tania Emi, Tanner Barnes, Emma Orton, Society for Biomaterials annual meeting and exposition . 2018

机译：磁响应水凝胶可优化抗癌治疗的给药方式
5. Ab initio Prediction of Reduction Potentials of Pharmaceutically Relevant 3-Aryl-Quinoxaline-2-carbonitrile 1,4-di-N-oxide Derivatives [D] . Miller, Eric M. 2018

机译：AB Initio对药学相关的3-芳基 - 喹喔啉-2-腈1,4-Di-N-氧化物衍生物的降低电位的预测
6. Esters of Quinoxaline 1ˏ4-Di-N-oxide with Cytotoxic Activity on Tumor Cell Lines Based on NCI-60 Panel [O] . Gildardo Rivera, Syed Shoaib Ahmad Shah, Daniel Arrieta-Baez, 2017

机译：基于NCI-60面板的具有细胞毒性活性的喹喔啉1oxide4-Di-N-氧化物的酯
7. Enzyme-Activated, Hypoxia-Selective DNA Damage by 3-Amino-2- quinoxalinecarbonitrile 1, 4-Di-N-oxide [O] . -1

机译：酶活化，缺氧选择性DNA损伤3-氨基-2-喹喔啉羰基腈1,4-二氧化氮

New quinoxaline 1, 4-di-N-oxides: anticancer and hypoxia-selective therapeutic agents.

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