Novel erythromycin derivatives with aryl groups tethered to the C-6 position are potent protein synthesis inhibitors and active against multidrug-resistant respiratory pathogens.

Ma Z; bbott.com; Clark RF; Brazzale A; Wang S; Rupp MJ; Li L; Griesgraber G; Zhang S; Yong H; Phan LT; Nemoto PA; Chu DT; Plattner JJ; Zhang X; Zhong P; Cao Z; Nilius AM; Shortridge VD; Flamm R; Mitten M; Meulbroek J; Ewing P; Alder J; Or YS

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Novel erythromycin derivatives with aryl groups tethered to the C-6 position are potent protein synthesis inhibitors and active against multidrug-resistant respiratory pathogens.

机译：具有连接至C-6位置的芳基的新型红霉素衍生物是有效的蛋白质合成抑制剂，可有效抵抗多种药物引起的呼吸道病原体。

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A novel series of erythromycin derivatives has been discovered with potent activity against key respiratory pathogens, including those resistant to erythromycin. These compounds are characterized by having an aryl group tethered to the C-6 position of the erythronolide skeleton. Extensive structural modification of the C-6 moiety led to the discovery of several promising compounds with potent activity against both mef- and erm-mediated resistant Streptoccoccus pneumoniae. Preliminary mechanistic studies indicated that the new macrolides are potent protein synthesis inhibitors, which interact with methylated ribosomes isolated from resistant organisms. In experimental animal models, these compounds exhibited excellent in vivo efficacy and balanced pharmacokinetic profiles.

机译：已经发现了一系列新的红霉素衍生物，它们对关键的呼吸道病原体具有有效的活性，包括对红霉素具有抗性的病原体。这些化合物的特征在于具有连接至赤藓醇内酯骨架的C-6位的芳基。 C-6部分的广泛结构修饰导致发现了几种具有前景的化合物，这些化合物具有针对mef和erm介导的耐药性肺炎链球菌的有效活性。初步的机理研究表明，新的大环内酯类是有效的蛋白质合成抑制剂，可与从抗性生物体中分离出的甲基化核糖体相互作用。在实验动物模型中，这些化合物表现出出色的体内功效和平衡的药代动力学特征。

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来源
《Journal of Medicinal Chemistry》 |2001年第24期|共20页
作者
Ma Z; bbott.com; Clark RF; Brazzale A; Wang S; Rupp MJ; Li L; Griesgraber G; Zhang S; Yong H; Phan LT; Nemoto PA; Chu DT; Plattner JJ; Zhang X; Zhong P; Cao Z; Nilius AM; Shortridge VD; Flamm R; Mitten M; Meulbroek J; Ewing P; Alder J; Or YS;
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正文语种 eng
中图分类药学;
关键词
Protein Synthesis Inhibitors; 蛋白质合成抑制药;

机译：Protein Synthesis Inhibitors;蛋白质合成抑制药;

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1. Novel erythromycin derivatives with aryl groups tethered to the C-6 position are potent protein synthesis inhibitors and active against multidrug-resistant respiratory pathogens. [J] . Ma Z, bbott.com, Clark RF, Journal of Medicinal Chemistry . 2001,第24期

机译：具有连接至C-6位置的芳基的新型红霉素衍生物是有效的蛋白质合成抑制剂，可有效抵抗多种药物引起的呼吸道病原体。
2. Novel 4-anilinoquinazolines with C-6 carbon-linked side chains: synthesis and structure-activity relationship of a series of potent, orally active, EGF receptor tyrosine kinase inhibitors. [J] . Hennequin LF, Ballard P, Boyle FT, Bioorganic and Medicinal Chemistry Letters . 2006,第10期

机译：具有C-6碳连接侧链的新型4-苯胺基喹唑啉：一系列有效的，口服活性EGF受体酪氨酸激酶抑制剂的合成与构效关系。
3. 4''-O-(omega-Quinolylamino-alkylamino)propionyl derivatives of selected macrolides with the activity against the key erythromycin resistant respiratory pathogens. [J] . Fajdetic A, Cipcic Paljetak H, Lazarevski G, Bioorganic and medicinal chemistry . 2010,第17期

机译：4' - O-（Omega-喹啉基氨基 - 烷基氨基）选定的大溴化胶酶的丙酰基衍生物，其活性抵抗关键的红霉素抗性呼吸道病原体。
4. Molecular Docking Analysis of Podophyllotoxin Derivatives in Sulawesi Propolis as Potent Inhibitors of Protein Kinases [C] . Darin Flamandita, Kenny Lischer, Diah Kartika Pratami, International Symposium on Sustainable and Clean Energy;International Conference on Quality in Research . 2020

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Novel erythromycin derivatives with aryl groups tethered to the C-6 position are potent protein synthesis inhibitors and active against multidrug-resistant respiratory pathogens.

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