Continued exploration of the triazolopyridine scaffold as a platform for p38 MAP kinase inhibition.

Jerome KD; Rucker PV; Xing

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Continued exploration of the triazolopyridine scaffold as a platform for p38 MAP kinase inhibition.

机译：继续探索三唑并吡啶支架作为p38 MAP激酶抑制的平台。

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The structure based drug design, synthesis and structure-activity relationship of a series of C6 sulfur linked triazolopyridine based p38 inhibitors are described. The metabolic deficiencies of this series were overcome through changes in the C6 linker from sulfur to methylene, which was predicted by molecular modeling to be bioisosteric. X-ray of the ethylene linked compound 61 confirmed the predicted binding orientation of the scaffold in the p38 enzyme.

机译：描述了一系列基于C6硫连接的三唑并吡啶基的p38抑制剂的基于结构的药物设计，合成和构效关系。通过从硫到亚甲基的C6接头变化克服了该系列的代谢缺陷，这通过分子模型预测是生物等排的。乙烯连接的化合物61的X射线证实了支架在p38酶中的预期结合方向。

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《Bioorganic and Medicinal Chemistry Letters》 |2010年第2期|共5页
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Jerome KD; Rucker PV; Xing;
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1. Continued exploration of the triazolopyridine scaffold as a platform for p38 MAP kinase inhibition. [J] . Jerome KD, Rucker PV, Xing Bioorganic and Medicinal Chemistry Letters . 2010,第2期

机译：继续探索三唑并吡啶支架作为p38 MAP激酶抑制的平台。
2. Insight into the structural determinants of imidazole scaffold-based derivatives as P38 MAP kinase inhibitors by computational explorations [J] . Current medicinal chemistry . 2012,第23期

机译：通过计算探索洞察咪唑支架基衍生物作为P38 MAP激酶抑制剂的结构决定因素
3. CoMFA and docking studies on triazolopyridine oxazole derivatives as p38 MAP kinase inhibitors. [J] . Shashi-Nayana MR, Sekhar YN, Siva-Kumari N, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2008,第6期

机译：CoMFA和三唑并吡啶恶唑衍生物作为p38 MAP激酶抑制剂的对接研究。
4. Phosphorylation and Activation of 5-Lipoxvgen ase by P38 Kinase-Activated MAPKAP Kinases [C] . Oliver Werz, Jenny Klemm, Olof Radmark, International Stereotactic Radiosurgery Society . 2000

机译：P38激酶活化MapKap激酶的磷酸化和5-脂糖尿病ASE的活化
5. Impact of Redox Modifications on p38α MAP Kinase Global Substrate Selection [D] . Hampton, Laquaundra. 2019

机译：氧化还原修饰对p38αMAP激酶整体底物选择的影响
6. Proteasome inhibitors up-regulate haem oxygenase-1 gene expression: requirement of p38 MAPK (mitogen-activated protein kinase) activation but not of NF-kappaB (nuclear factor kappaB) inhibition. [O] . Wen-Tung Wu, Kwan-Hwa Chi, Feng-Ming Ho, 2004

机译：蛋白酶体抑制剂上调血红素加氧酶-1基因表达：需要激活p38 MAPK（促分裂原激活的蛋白激酶）而不需要抑制NF-κB（核因子κB）。
7. SB202190-induced cell type-specific vacuole formation and defective autophagy do not depend on p38 MAP kinase inhibition. [O] . Manoj B Menon, Alexey Kotlyarov, Matthias Gaestel 2011

机译：sB202190诱导的细胞类型特异性液泡形成和缺陷自噬不依赖于p38 map激酶抑制。

Continued exploration of the triazolopyridine scaffold as a platform for p38 MAP kinase inhibition.

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