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羧基末端残基的缺失破坏了两亲性抗菌肽氨基末端的折叠、自缔合和热稳定性。

Deletion of the carboxyl-terminal residue disrupts the amino-terminal folding, self-association, and thermal stability of an amphipathic antimicrobial peptide.

机构信息

Department of Chemistry, Tamkang University, No.151 Yingzhuan Road, Tamsui District, New Taipei City, 25137, Taiwan, China.

出版信息

J Pept Sci. 2014 Jun;20(6):438-45. doi: 10.1002/psc.2635. Epub 2014 Apr 24.

DOI:10.1002/psc.2635
PMID:24764036
Abstract

Understanding the complex relationship between amino acid sequence and protein behaviors, such as folding and self-association, is a major goal of protein research. In the present work, we examined the effects of deleting a C-terminal residue on the intrinsic properties of an amphapathic α-helix of mastoparan-B (MP-B), an antimicrobial peptide with the sequence LKLKSIVSWAKKVL-NH2. We used circular dichroism and nuclear magnetic resonance to demonstrate that the peptide MP-B([1-13]) displayed significant unwinding at the N-terminal helix compared with the parent peptide of MP-B, as the temperature increased when the residue at position 14 was deleted. Pulsed-field gradient nuclear magnetic resonance data revealed that MP-B forms a larger diffusion unit than MP-B([1-13]) at all experimental temperatures and continuously dissociates as the temperature increases. In contrast, the size of the diffusion unit of MP-B([1-13]) is almost independent of temperature. These findings suggest that deleting the flexible, hydrophobic amino acid from the C-terminus of MP-B is sufficient to change the intrinsic helical thermal stability and self-association. This effect is most likely because of the modulation of enthalpic interactions and conformational freedom that are specified by this residue. Our results implicate terminal residues in the biological function of an antimicrobial peptide.

摘要

了解氨基酸序列与蛋白质行为(如折叠和自组装)之间的复杂关系,是蛋白质研究的主要目标。在本工作中,我们研究了删除 C 末端残基对抗菌肽 mastoparan-B(MP-B)的两性α-螺旋固有性质的影响,其序列为 LKLKSIVSWAKKVL-NH2。我们使用圆二色性和核磁共振证明,与 MP-B 的母体肽相比,当位置 14 的残基被删除时,肽 MP-B([1-13])在 N 端螺旋处显示出明显的解旋,随着温度升高。脉冲场梯度核磁共振数据显示,在所有实验温度下,MP-B 形成的扩散单元大于 MP-B([1-13]),并且随着温度升高而连续解离。相比之下,MP-B([1-13])的扩散单元大小几乎与温度无关。这些发现表明,从 MP-B 的 C 末端删除柔性疏水性氨基酸足以改变其内在的螺旋热稳定性和自组装。这种影响很可能是由于该残基调节了焓相互作用和构象自由度。我们的结果表明末端残基在抗菌肽的生物学功能中起作用。

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Deletion of the carboxyl-terminal residue disrupts the amino-terminal folding, self-association, and thermal stability of an amphipathic antimicrobial peptide.羧基末端残基的缺失破坏了两亲性抗菌肽氨基末端的折叠、自缔合和热稳定性。
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