首页> 外文期刊>Peptides: An International Journal >Antimicrobial properties of the frog skin peptide, ranatuerin-1 and its (Lys-8)-substituted analog.
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Antimicrobial properties of the frog skin peptide, ranatuerin-1 and its (Lys-8)-substituted analog.

机译:青蛙皮肤肽,ranatuerin-1及其(Lys-8)取代类似物的抗菌特性。

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摘要

The predicted conformation of ranatuerin-1 (SMLSVLKNLG(10)KVGLGFVACK(20)INK QC), an antimicrobial peptide first isolated from the skin of the bullfrog Rana catesbeiana, comprises three structural domains: alpha-helix (residues 1-8), beta-sheet (residues 11-16) and beta-turn (residues 20-25). Circular dichroism studies confirm significant alpha-helical character in 50% trifluoroethanol. Replacement of Cys-19 and Cys-25 by serine resulted only in decreased antimicrobial potency but deletion of either the cyclic heptapeptide region [residues (19-25)] or the N-terminal domain [residues (1-8)] produced inactive analogs. Substitution of the glycine residues in the central domain of the [Ser-19, Ser-25] analog by lysine produced inactive peptides despite increased alpha-helical content and cationicity. The substitution Asn-8-->Lys gave a ranatuerin-1 analog with increased alpha-helicity and cationicity and increased potency against a range of Gram-positive and Gram-negative bacteria and against C. albicans but only a small increase (21%) in hemolytic activity. In contrast, increasing alpha-helicity and hydrophobicity by the substitution Asn-22-->Ala resulted in a 3.5-fold increase in hemolytic activity. Effects on antimicrobial potencies of substitutions of neutral amino acids at positions 4, 18, 22, and 24 by lysine were less marked. Strains of pathogenic E. coli from different groups showed varying degrees of sensitivity to ranatuerin-1 (MIC between 5 and 40 microM) but [Lys-8] ranatuerin-1 showed increased potency (between 2- and 8-fold; P < 0.01) against all strains. The data demonstrate that [Lys-8] ranatuerin-1 shows potential as a candidate for drug development.
机译:ranatuerin-1(SMLSVLKNLG(10)KVGLGFVACK(20)INK QC)的预测构象,一种抗菌肽,首先从牛蛙Rana catesbeiana的皮肤中分离,包含三个结构域:α-螺旋(残基1-8),β -页(残基11-16)和β-转弯(残基20-25)。圆二色性研究证实,在50%三氟乙醇中有明显的α-螺旋特征。用丝氨酸替代Cys-19和Cys-25只会降低抗菌效力,但会删除环状七肽区域[残基(19-25)]或N末端结构域[残基(1-8)]产生的失活类似物。尽管增加了α-螺旋含量和阳离子度,但是赖氨酸取代[Ser-19,Ser-25]类似物中央结构域中的甘氨酸残基产生了无活性的肽。取代Asn-8-> Lys产生了ranatuerin-1类似物,具有增加的α-螺旋性和阳离子性,并且对一系列革兰氏阳性和革兰氏阴性细菌以及白色念珠菌具有增强的效力,但仅增加很小一部分(21% )的溶血活性。相反,通过取代Asn-22-> Ala来增加α-螺旋性和疏水性会导致溶血活性增加3.5倍。赖氨酸对第4、18、22和24位的中性氨基酸取代的抗菌效力的影响较小。来自不同组的致病性大肠杆菌菌株对ranatuerin-1的敏感性不同(MIC在5至40 microM之间),但是[Lys-8] ranatuerin-1的效力增强(2至8倍; P <0.01 )抵抗所有压力。数据表明[Lys-8] ranatuerin-1具有潜在的药物开发潜力。

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