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Design, synthesis, and antimicrobial activities of novel functional peptides against Gram-positive and Gram-negative bacteria

机译:对革兰氏阳性和革兰氏阴性细菌的新型功能肽的设计,合成和抗微生物活性

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摘要

The extensive use of antibiotics in medicine results in the multidrug resistance of bacteria, making the development of new antimicrobial agents an urgent need. Antimicrobial peptides (AMPs) are considered as a new class of antibiotic with characteristics including an ability to kill target cells rapidly and a broad spectrum of activity. We have developed a potent antimicrobial peptide MAP-0403 (MIC = 5 mu M), but it exhibited a high hemolytic side-effect (70.7%). To reduce its hemolytic effect and increase antimicrobial activity, three peptides derivatives of MAP-0403 (J-1, J-2, and J-3) were designed, synthesized by solid phase synthesis, purified by RP-HPLC, and characterized by MALDI-TOF MS. Structure-activity relationships of these peptides were studied by using circular dichroism and antimicrobial assays. The percentage of helical structure in J-1, J-2, and J-3 was lower than that of MAP-0403. The antimicrobial activity of J-1 was the same as that of MAP-0403 (MIC = 5 mu M), J-2 exhibited the highest activity (MIC = 2.5 mu M), while J-3 showed decreased activity (MIC = 10 mu M). Compared to MAP-0403, J-2 showed significantly reduced hemolytic effect (3.4%), while J-1 and J-3 showed slightly decreased hemolytic effect (46.2%, 55.6%, respectively). Peptide J-2 was discovered as a novel and potent antimicrobial agents.
机译:在医学中广泛使用抗生素导致细菌的多药抗性,使新的抗菌剂的发展迫切需要。抗微生物肽(AMPs)被认为是一种具有特征的新类抗生素,包括迅速杀死靶细胞的能力和广谱的活性。我们开发了有效的抗微生物肽图-0403(MIC =5μm),但它表现出高溶血性副作用(70.7%)。为了降低其溶血作用和增加抗微生物活性,通过固相合成合成,通过固相合成来设计三种肽衍生物,由RP-HPLC纯化,并以MALDI为特征-tof ms。通过使用圆形二色性和抗微生物测定来研究这些肽的结构活性关系。 J-1,J-2和J-3中的螺旋结构的百分比低于MAP-0403的百分比。 J-1的抗微生物活性与MAP-0403(MIC =5μm)相同,J-2表现出最高的活性(MIC =2.5μm),而J-3表现出降低的活性(MIC = 10 mu m)。与MAP-0403相比,J-2显示出显着降低的溶血效果(3.4%),而J-1和J-3显示出略微降低溶血作用(分别为46.2%,55.6%)。肽J-2被发现为新颖和有效的抗微生物剂。

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