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通过疏水和亲水氨基酸延伸来提高超短肽的抗菌活性和选择性。

Improving the antibacterial activity and selectivity of an ultra short peptide by hydrophobic and hydrophilic amino acid stretches.

机构信息

Department of Biochemistry, Faculty of Science, Khon Kaen University, Khon Kaen 40002, Thailand.

出版信息

Bioorg Med Chem Lett. 2013 Aug 15;23(16):4657-62. doi: 10.1016/j.bmcl.2013.06.005. Epub 2013 Jun 15.

Abstract

The principle of amino acid stretches tagged at the C terminal of Luecrocin I, which is an ultra-short antibacterial peptide, by tryptophan and arginine or lysine has been reported. The choice of amino acid type at each stretch position depends on the hydrophobic and hydrophilic regions visualized in the helical wheel pattern of Luecrocin I. Oligopeptide tagging should also consider the properties such as positive charge, hydrophobicity, the content of hydrophobic amino acids, polar angle, the properly hydrophilic and hydrophobic facets. Amidation at C terminal and lysine substitute for arginine can increase selectivity between mammalian cells (hemolytic and MTT assay) and bacterial cells tested. KT2 and RT2 which have 53% hydrophobic residues, 7 positive charges, 160° polar angle, -0.02 (KT2) and -0.04 (RT2) hydrophobicity were effective against S. typhi DMST 22842, S. epidermidis ATCC 12228, E. coli ATCC 25922 and V. cholerae non-O1, non-O139. The SEM images implied that the antibacterial mechanism of RT2 and KT2 may depend on concentration rather than time. Finally, RT2 and KT2 can be new antibacterial agents or may be further developed for alternative antibiotics.

摘要

已报道了在超短抗菌肽 Luecrocin I 的 C 末端通过色氨酸和精氨酸或赖氨酸进行氨基酸延伸标记的原理。每个延伸位置的氨基酸类型的选择取决于 Luecrocin I 螺旋轮图案中可视化的疏水区和亲水区。寡肽标记还应考虑正电荷、疏水性、疏水性氨基酸含量、极性角、适当的亲水性和疏水性方面等特性。C 末端酰胺化和赖氨酸取代精氨酸可以提高哺乳动物细胞(溶血和 MTT 测定)和测试细菌细胞之间的选择性。具有 53%疏水性残基、7 个正电荷、160°极性角、-0.02(KT2)和-0.04(RT2)疏水性的 KT2 和 RT2 对 S. typhi DMST 22842、S. epidermidis ATCC 12228、E. coli ATCC 25922 和 V. cholerae non-O1、非-O139 有效。SEM 图像表明,RT2 和 KT2 的抗菌机制可能取决于浓度而不是时间。最后,RT2 和 KT2 可以成为新的抗菌剂,或者可能进一步开发为替代抗生素。

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