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具有潜在抗菌活性的prenylated flavonoids:合成、生物活性和计算机研究。

Prenylated Flavonoids with Potential Antimicrobial Activity: Synthesis, Biological Activity, and In Silico Study.

机构信息

Laboratorio de Productos Naturales, Departamento de Química, Universidad Técnica Federico Santa María, Valparaíso 2390123, Chile.

Centro de Biotecnología CB-DAL, Universidad Técnica Federico Santa María, Valparaíso 2390136, Chile.

出版信息

Int J Mol Sci. 2021 May 22;22(11):5472. doi: 10.3390/ijms22115472.

Abstract

Prenylated flavonoids are an important class of naturally occurring flavonoids with important biological activity, but their low abundance in nature limits their application in medicines. Here, we showed the hemisynthesis and the determination of various biological activities of seven prenylated flavonoids, named , with an emphasis on antimicrobial ones. Compounds , , and showed inhibitory activity against human pathogenic fungi. Compounds , (flavanones) and (isoflavone) were the most active against clinical isolated MRSA, showing that structural requirements as prenylation at position C-6 or C-8 and OH at positions C-5, 7, and 4' are key to the antibacterial activity. The combination of or with commercial antibiotics synergistically enhanced the antibacterial activity of vancomycin, ciprofloxacin, and methicillin in a factor of 10 to 100 times against drug-resistant bacteria. Compound combined with ciprofloxacin was able to decrease the levels of ROS generated by ciprofloxacin. According to docking results of enantiomer of with ATP-binding cassette transporter showed the most favorable binding energy; however, more studies are needed to support this result.

摘要

烯丙基化黄酮类化合物是一类重要的天然黄酮类化合物,具有重要的生物活性,但由于其在自然界中的含量较低,限制了其在药物中的应用。在这里,我们展示了七种烯丙基化黄酮类化合物(命名为 )的半合成及其各种生物活性的测定,重点是抗菌活性。化合物 、 和 对人体致病真菌具有抑制活性。化合物 、 (黄烷酮)和 (异黄酮)对临床分离的 MRSA 最具活性,表明 C-6 或 C-8 位的烯丙基化和 C-5、7 和 4'位的 OH 是抗菌活性的关键结构要求。或 与商业抗生素联合使用可协同增强万古霉素、环丙沙星和甲氧西林对耐药菌的抗菌活性 10 至 100 倍。化合物 与环丙沙星联合使用能够降低环丙沙星产生的 ROS 水平。根据与 ATP 结合盒转运蛋白结合的 对映异构体的对接结果显示出最有利的结合能;然而,还需要更多的研究来支持这一结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1815/8196815/cb62d5960980/ijms-22-05472-sch001.jpg

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