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理解糖基化苏氨酸和富含脯氨酸的抗菌肽 Drosocin 的立体专一性作用的重要性。

Understanding the importance of glycosylated threonine and stereospecific action of Drosocin, a Proline rich antimicrobial peptide.

机构信息

Structural Biology Unit, National Institute of Immunology, Aruna Asaf Ali Marg, New Delhi 110 067, India.

Structural Biology Unit, National Institute of Immunology, Aruna Asaf Ali Marg, New Delhi 110 067, India.

出版信息

Eur J Med Chem. 2015 Mar 6;92:637-47. doi: 10.1016/j.ejmech.2015.01.032. Epub 2015 Jan 16.

DOI:10.1016/j.ejmech.2015.01.032
PMID:25617693
Abstract

Glycosylation is an essential post-translational modification for few antimicrobial peptides of Proline rich class. In the present study we have shown the importance of Thr glycosylation over Ser glycosylation in Drosocin. Difference of a methyl group makes glycosylated-Thr preferred over glycosylated-Ser and renders higher activity to the peptide, probably due to the rigid conformation provided by the glycosylated-Thr. The structural rigidity provided by glycosylated-Thr to Drosocin backbone was mimicked by substituting glycosylated-Thr11, Ser7 and Ser12 with Pro residues. The designed non-glycosylated analogue, P(7)P(11)P(12)-Drosocin, exhibited functional and structural properties similar to that of the native monoglycosylated peptide. The functional importance of stereospecificity of amino acids and sugar was further explored. Interestingly, (all D) p(7)p(11)p(12)-Drosocin failed to exhibit antimicrobial activity but had comparable binding affinity to DnaK, one of the proposed targets for Proline rich class of antibacterial peptides, as that of its L counterpart. However, Drosocin containing either L or D enantiomeric sugar, displayed antimicrobial activity and binding affinity to bacterial heat shock protein, DnaK. The flow cytometry (FACS) experiments revealed the internalization of Drosocins bearing enantiomeric sugars and P(7)P(11)P(12)-Drosocin but not of its d-enantiomer into bacteria suggesting the importance of stereospecificity of amino acids for membrane entry. Once internalized both enantiomeric peptides may behave similarly. This assumption was corroborated by in vitro activity of (all D) p(7)p(11)p(12)-Drosocin in cell free assay where it abrogated transcription/translation pathway similar to l-enantiomer but could not inhibit the same in whole cell assay. These research findings provide insights into the mode of action of Proline rich class of antibacterial peptides and guidelines for designing functionally equivalent non-glycosylated analogues of glycosylated antibacterial peptides.

摘要

糖基化是富含脯氨酸的几类抗菌肽的一种重要的翻译后修饰。在本研究中,我们表明了 Drosocin 中 Thr 糖基化相对于 Ser 糖基化的重要性。一个甲基的差异使得糖基化-Thr 优先于糖基化-Ser,并赋予肽更高的活性,这可能是由于糖基化-Thr 提供了刚性构象。通过用脯氨酸残基取代糖基化-Thr11、Ser7 和 Ser12,模拟了糖基化-Thr 赋予 Drosocin 骨架的结构刚性。设计的非糖基化类似物 P(7)P(11)P(12)-Drosocin 表现出与天然单糖基化肽相似的功能和结构特性。进一步探讨了氨基酸和糖的立体特异性的功能重要性。有趣的是,(all D)p(7)p(11)p(12)-Drosocin 没有表现出抗菌活性,但与富含脯氨酸的抗菌肽的一个假定靶标 DnaK 的结合亲和力与 L 对相似。然而,含有 L 或 D 对映异构体糖的 Drosocin 都表现出抗菌活性和与细菌热休克蛋白 DnaK 的结合亲和力。流式细胞术(FACS)实验表明,含有对映异构体糖和 P(7)P(11)P(12)-Drosocin 的 Drosocins 以及 P(7)P(11)P(12)-Drosocin 的 d-对映体都能进入细菌内部,这表明氨基酸的立体特异性对膜进入很重要。一旦进入细胞,两种对映异构体的肽可能表现相似。这一假设得到了在无细胞测定中(all D)p(7)p(11)p(12)-Drosocin 的体外活性的证实,它与 L-对映体相似地阻断转录/翻译途径,但在全细胞测定中不能抑制相同途径。这些研究结果为富含脯氨酸的抗菌肽的作用模式提供了深入了解,并为设计功能等效的非糖基化类似物提供了指导。

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