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论蛋清溶菌酶新的非催化抗菌功能:一种构象依赖性活性。

On the novel catalytically-independent antimicrobial function of hen egg-white lysozyme: a conformation-dependent activity.

作者信息

Ibrahim H R

机构信息

Kagoshima University, Faculty of Agriculture, Department of Biochemical Science and Technology, Japan.

出版信息

Nahrung. 1998 Aug;42(3-4):187-93. doi: 10.1002/(sici)1521-3803(199808)42:03/04<187::aid-food187>3.3.co;2-6.

DOI:10.1002/(sici)1521-3803(199808)42:03/04<187::aid-food187>3.3.co;2-6
PMID:9739565
Abstract

Dependency of the antimicrobial activity on the conformation of lysozme was examined by the means of gradual thermal inactivation at neutral pH and different temperatures. We found that heating of lysozyme at increasing temperatures for 20 min in pH 6.0 results in progressive loss of enzyme activity, while greatly promotes its antimicrobial action to the Gram-negative bacteria without a detrimental effect on the inherent bactericidal activity to Gram-positive ones, suggesting action independent of catalytic function. The most potent bactericidal conformation of lysozyme to either Gram-negative or -positie bacteria was that retaining approximately 50% of the native enzyme activity (HL80/6). HL80/6 showed several fold increase in surface hydrophobicity, with exposed two thiol groups, and 17% deamidation. Spectrophotometric analysis of HL80/6 revealed slight changes in its secondary structures, but considerable global conformational changes as a result of the formation of beta conformation, via cyclic imide, at the three aspartylglycyl sequences of lysozyme molecule. Direct damage to the bacertial membranes by HL80/6, was demonstrated by using ELISA and liposomal membrane model. Furthermore, the antimicrobial activity of HL80/6 was inhibited by the divalent cations Ca2+ and Mg2+ suggesting that HL80/6 interacts at a divalent cation binding site on the bacterial membrane and subsequently permeabilize it. The results introduce an interesting structure-antimicrobial relationship that the antimicrobial action of lysozyme is independent of its catalytic function. In addition, it is worth emphasizing that the naturally-occurring conformational transition of lysozyme at physiological temperatures can be a biologically relevant event to switch its antimicrobial specificity to include the food-borne pathogens and heralding fascinating opportunities for application in formulated food systems.

摘要

通过在中性pH值和不同温度下逐步热失活的方法,研究了溶菌酶抗菌活性对其构象的依赖性。我们发现,在pH 6.0条件下,随着温度升高对溶菌酶加热20分钟会导致酶活性逐渐丧失,同时极大地促进其对革兰氏阴性菌的抗菌作用,而对其对革兰氏阳性菌的固有杀菌活性没有不利影响,这表明其作用独立于催化功能。溶菌酶对革兰氏阴性菌或阳性菌最有效的杀菌构象是保留约50%天然酶活性的构象(HL80/6)。HL80/6的表面疏水性增加了几倍,有两个巯基暴露,脱酰胺率为17%。对HL80/6的分光光度分析显示其二级结构有轻微变化,但由于溶菌酶分子的三个天冬氨酰甘氨酰序列通过环状酰亚胺形成β构象,导致整体构象发生了相当大的变化。通过酶联免疫吸附测定(ELISA)和脂质体膜模型证明了HL80/6对细菌膜的直接损伤。此外,HL80/6的抗菌活性受到二价阳离子Ca2+和Mg2+的抑制,这表明HL80/6在细菌膜上的二价阳离子结合位点相互作用,随后使其通透性增加。这些结果引入了一种有趣的结构-抗菌关系,即溶菌酶的抗菌作用独立于其催化功能。此外,值得强调的是,溶菌酶在生理温度下自然发生的构象转变可能是一个生物学相关事件,可将其抗菌特异性转变为包括食源性病原体,并为在配方食品系统中的应用带来迷人的机会。

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