Parmar Anish, Iyer Abhishek, Lloyd Daniel G, Vincent Charlotte S, Prior Stephen H, Madder Annemieke, Taylor Edward J, Singh Ishwar
School of Pharmacy, JBL Building, University of Lincoln, Beevor St. Lincoln, LN67DL, UK.
Chem Commun (Camb). 2017 Jul 6;53(55):7788-7791. doi: 10.1039/c7cc04021k.
The recently discovered cyclic depsipeptide, teixobactin, is a highly potent antibiotic against multi-drug resistant pathogens such as methicillin-resistant Staphylococcus aureus (MRSA) and Mycobaterium tuberculosis. It comprises of 4 D amino acids and a rare l-allo-enduracididine amino acid. The synthesis of a properly protected l-allo-enduracididine amino acid and its incorporation into teixobactin is time consuming, synthetically challenging and low yielding and is therefore a major bottleneck in the development of potent analogues of teixobactin. In this article, we have synthesised 8 analogues of teixobactin using commercially available building blocks by replacing the l-allo-enduracididine amino acid with its isosteres. Furthermore, we have tested all the compounds against a panel of Gram positive bacteria including MRSA and explained the observed trend in biological activity. Although all the analogues were active, three analogues from this work, showed very promising activity against MRSA (MIC 1 μg mL). We can conclude that amino acids which are the closest isosteres of l-allo-enduracididine are the key to synthesising simplified potent analogues of teixobactin using rapid syntheses and improved yields.
最近发现的环缩酚酸肽类抗生素——替考拉宁,是一种对耐多药病原体(如耐甲氧西林金黄色葡萄球菌(MRSA)和结核分枝杆菌)具有高效抗菌活性的抗生素。它由4个D型氨基酸和1个罕见的L-别-恩杜拉西定氨基酸组成。合成一个经过适当保护的L-别-恩杜拉西定氨基酸并将其纳入替考拉宁的过程耗时、合成难度大且产率低,因此是开发替考拉宁有效类似物的主要瓶颈。在本文中,我们使用市售的构建模块,通过用其电子等排体取代L-别-恩杜拉西定氨基酸,合成了8种替考拉宁类似物。此外,我们对所有化合物针对包括MRSA在内的一组革兰氏阳性菌进行了测试,并解释了观察到的生物活性趋势。尽管所有类似物都具有活性,但这项工作中的三种类似物对MRSA表现出非常有前景的活性(最低抑菌浓度为1μg/mL)。我们可以得出结论,与L-别-恩杜拉西定最接近的电子等排体氨基酸是使用快速合成方法和提高产率来合成简化的替考拉宁有效类似物的关键。
