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Effect of N- and C-Terminal Modifications on Cytotoxic Properties of Antimicrobial Peptide Tachyplesin I

机译:N-和C末端改性对抗菌肽Tachyplesin的细胞毒性特性的影响

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We analyze the effects of N-terminal acetylation and C-terminal amidation on the cytotoxic properties of beta-hairpin antimicrobial peptide tachyplesin I. MTT-assay showed that modified tachyplesin I exhibited increased cytotoxicity toward both tumor and normal human cells. Hemolytic activity of modified tachyplesin I was also higher than that of the initial molecule. In contrast to non-modified tachyplesin I, the peptide with C- and N-terminal modifications is resistant to proteolytic degradation in fresh human serum. C- and N-terminal modifications make tachyplesin I more attractive prototype of anticancer drug due to its more potent cytotoxic effect and better pharmacokinetic properties.
机译:我们分析N-末端乙酰化和C末端酰胺对β-发夹抗微生物肽TachypessI的细胞毒性特性的影响。MTT-assay显示,改性的TachypleSin I表现出朝向肿瘤和正常人体细胞的细胞毒性增加。 改性Tachyplesin I的溶血活性也高于初始分子的溶血活性。 与未修饰的TachypleSI相反,具有C-和N-末端修饰的肽对新鲜人血清的蛋白水解降解抗性。 C-和N-末端修饰使TachypleSin I具有更有吸引力的抗癌药物原型,由于其更有效的细胞毒性效果和更好的药代动力学性质。

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