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Rhodium(II) Proximity-Labeling Identifies a Novel Target Site on STAT3 for Inhibitors with Potent Anti-Leukemia Activity

机译：铑（II）贴近标签标识了STAT3上新型具有抗白血病活性的抑制剂的目标位点

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Nearly 40 % of children with acute myeloid leukemia (AML) suffer relapse arising from chemoresistance, often involving upregulation of the oncoprotein STAT3 (signal transducer and activator of transcription 3). Herein, rhodium(II)-catalyzed, proximity-driven modification identifies the STAT3 coiled-coil domain (CCD) as a novel ligand-binding site, and we describe a new naphthalene sulfonamide inhibitor that targets the CCD, blocks STAT3 function, and halts its disease-promoting effects in vitro, in tumor growth models, and in a leukemia mouse model, validating this new therapeutic target for resistant AML.

机译：急性髓细胞性白血病（AML）儿童中有近40％的人因化学抗药性而复发，通常涉及癌蛋白STAT3（信号转导子和转录激活子）3的上调。在本文中，铑（II）催化的邻近驱动修饰将STAT3卷曲螺旋结构域（CCD）识别为一个新的配体结合位点，并且我们描述了一种靶向CCD的新型萘磺酰胺抑制剂，可阻断STAT3功能并停止它在肿瘤生长模型和白血病小鼠模型中具有促进疾病的作用，从而验证了抗AML的这一新治疗靶点。

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Minus Matthew B.; Liu Wei; Vohidov Farrukh; Kasembeli Moses M.; Long Xin; Krueger Michael; Stevens Alexandra; Kolosov Mikhail I.; Tweardy David J.; Sison Edward Allen R.; Redell Michele S.; Ball Zachary T;
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年度 2015
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1. Rhodium(II) Proximity-Labeling Identifies a Novel Target Site on STAT3 for Inhibitors with Potent Anti-Leukemia Activity [J] . Minus Matthew B., Liu Wei, Vohidov Farrukh, Angewandte Chemie . 2015,第44期

机译：铑（II）贴近标签标识了STAT3上新型具有抗白血病活性的抑制剂的目标位点
2. COMPUTER-AIDED SCREENING IDENTIFIED A NOVEL SMALL INHIBITOR THAT DISPLAYS POTENT ANTI-MYELOMA ACTIVITY BY SUPPRESSING CONSTITUTIVE AND INTERLEUKIN-6-TRIGGERED JAK2-STAT3 ACTIVATION [J] . Experimental Hematology: Official Publication of the International Society for Experimental Hematology . 2013,第8Suppla1期

机译：计算机辅助筛选通过抑制本构和白介素6触发的JAK2-STAT3激活，显示了一种新型的小抑制剂，该抑制剂可显示潜在的抗骨髓瘤活性
3. Identifying New Drug Targets for Potent Phospholipase D Inhibitors: Combining Sequence Alignment, Molecular Docking, and Enzyme Activity/Binding Assays [J] . Djakpa Helene, Kulkarni Aditya, Barrows-Murphy Scheneque, Chemical biology and drug design . 2016,第5期

机译：确定有效的磷脂酶D抑制剂的新药靶点：组合序列比对，分子对接和酶活性/结合测定
4. Mass Spectrometry Investigation of the Binding Sites of a Small-Molecule STAT3-STAT3 Inhibitor [C] . Sibylle Heidelberger, Giovanna Zinzalla, Dyeison Antonow, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2012

机译：小分子Stat3-Stat3抑制剂结合位点的质谱研究
5. P27 as a molecular target for cancer therapeutics: Discovering small molecule inhibitors of p27 proteolysis and structure-activity relationship and mechanistic studies of largazole, a potent inhibitor of histone deacetylase . [D] . Ungermannova, Dana. 2010

机译：P27作为癌症治疗的分子靶标：发现p27蛋白水解和结构活性关系的小分子抑制剂以及组蛋白脱乙酰基酶的有效抑制剂largazole的机理研究。
6. Rhodium(II) proximity-labeling identifies a novel target site on STAT3 for inhibitors with potent anti-leukemia activity [O] . Matthew B. Minus, Dr. Wei Liu, Farrukh Vohidov, -1

机译：铑（II）邻近标记为具有有效抗白血病活性的抑制剂确定了STAT3上的新靶位
7. Drug-repositioning screening identified piperlongumine as a direct STAT3 inhibitor with potent activity against breast cancer [O] . U Bharadwaj, T K Eckols, M Kolosov, 2014

机译：药物重新定位筛选鉴定哌琅，作为直接STAT3抑制剂，具有抗乳腺癌的有效活性

Rhodium(II) Proximity-Labeling Identifies a Novel Target Site on STAT3 for Inhibitors with Potent Anti-Leukemia Activity

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