Improved Synthesis of MDL 73811-A Potent AdoMetDC Inhibitor and Anti-Trypanosomal Compound

Brockway Anthony J.; Cosner Casey C.; Volkov Oleg A.; Phillips Margaret A.; De Brabander Jef K.

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Improved Synthesis of MDL 73811-A Potent AdoMetDC Inhibitor and Anti-Trypanosomal Compound

机译：MDL 73811-A强力AdoMetDC抑制剂和抗锥虫类化合物的合成方法改进

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An improved synthesis of MDL 73811 - a potent AdoMetDC (S-adenosylmethionine decarboxylase) inhibitor and anti-trypanosomal compound with in vivo activity - has been completed in four steps from commercially available 2',3'-O-isopropylideneadenosine. Utilization of Mitsunobu chemistry was crucial for the reliable and scalable introduction of the 5'-methylamine moiety, which was problematic using traditional activation/displacement chemistry as previously reported. All reactions in this synthesis were run on gram-scale resulting in a five-fold increase in yield over the original synthesis.

机译：MDL 73811（一种有效的AdoMetDC（S-腺苷甲硫氨酸脱羧酶）抑制剂和具有体内活性的抗锥虫类化合物）的改良合成已由市售2'，3'-O-异丙基亚氨腺苷分四步完成。使用Mitsunobu化学方法对于5'-甲胺部分的可靠和可扩展引入至关重要，这是以前报道的使用传统活化/置换化学方法存在的问题。该合成中的所有反应均以克为单位进行，导致收率比原始合成提高了五倍。

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《Synthesis: International Journal of Methods in Synthetic Organic Chemistry》 |2016年第13期|共4页
作者
Brockway Anthony J.; Cosner Casey C.; Volkov Oleg A.; Phillips Margaret A.; De Brabander Jef K.;
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原文格式 PDF
正文语种 eng
中图分类化学;
关键词
nucleosides; drug discovery; Mitsunobu reaction; inhibitors; medicinal chemistry;

机译：核苷;药物发现;Mitsunobu反应;抑制剂;药物化学;
入库时间 2022-08-18 15:38:34

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1. Improved Synthesis of MDL 73811-A Potent AdoMetDC Inhibitor and Anti-Trypanosomal Compound [J] . Brockway Anthony J., Cosner Casey C., Volkov Oleg A., Synthesis: International Journal of Methods in Synthetic Organic Chemistry . 2016,第13期

机译：MDL 73811-A强力AdoMetDC抑制剂和抗锥虫类化合物的合成方法改进
2. The rational design of a novel potent analogue of the 5'-AMP-activated protein kinase inhibitor compound C with improved selectivity and cellular activity. [J] . Machrouhi F, Ouhamou N, Laderoute K, Bioorganic and Medicinal Chemistry Letters . 2010,第22期

机译：5'-AMP活化蛋白激酶抑制剂C具有改善的选择性和细胞活性的新型高效类似物的理性设计。
3. Synthesis and in silico studies of Novel Ru(II) complexes of Schiff base derivatives of 3-[(4-amino-5-thioxo-1,2,4-triazole-3-yl)methyl]-2(3H)-benzoxazolone compounds as potent Glutathione S-transferase and Cholinesterases Inhibitor [J] . Adiguzel Ragip, Turkan Fikret, Yildiko Umit, Journal of Molecular Structure . 2021,第1期

机译：三〜[（4-氨基-5-硫代-1,2,4-三唑-3-基）甲基] -2（3H） - 苯并恶唑酮的席夫碱衍生物的新型ru（II）复合物的合成及二氧化硅研究。-BenzoOxolone 化合物作为有效的谷胱甘肽S-转移酶和胆碱酯酶抑制剂
4. In silico identification of potent inhibitors of heat shoek protein 90(Hsp90)from Indonesian natural product compounds as a novel approach to treat ebola virus disease [C] . Muhammad Chandra Haikal, Mochammad Arfln Fardiansyah Nasution, Linggih Saputro Joint Conference on Chemistry . 2019

机译：从印度尼西亚天然产物化合物中硅质鉴定热沙蛋白90（HSP90）的有效抑制剂作为一种治疗埃博拉病毒疾病的新方法
5. Design, synthesis & evaluation of human Aurora kinase and phosphodiesterase inhibitors for anti-trypanosomal drug discovery via target repurposing. [D] . Ochiana, Stefan O. 2013

机译：设计，合成和评估人Aurora激酶和磷酸二酯酶抑制剂，通过靶标重新定位来抗锥虫药物。
6. Improved Synthesis of MDL 73811 – a Potent AdoMetDC Inhibitor and Anti-Trypanosomal Compound [O] . Anthony J. Brockway, Casey C. Cosner, Oleg A. Volkov, -1

机译：改进的MDL 73811的合成-一种有效的AdoMetDC抑制剂和抗锥虫类化合物
7. The rational design of a novel potent analogue of the 5′-AMP-activated protein kinase inhibitor compound C with improved selectivity and cellular activity [O] . Fouzia Machrouhi, Nouara Ouhamou, Keith Laderoute, 2010

机译：具有改进的选择性和细胞活性的5'-AMP活化蛋白激酶抑制剂C的新型有效类似物的理性设计

Improved Synthesis of MDL 73811-A Potent AdoMetDC Inhibitor and Anti-Trypanosomal Compound

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