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LanI-Mediated Lantibiotic Immunity in Bacillus subtilis: Functional Analysis

机译:LanI介导枯草芽孢杆菌的羊毛硫抗生素免疫:功能分析。

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Lantibiotics subtilin and nisin are produced by Bacillus subtilis and Lactococcus lactis, respectively. To prevent toxicity of their own lantibiotic, both bacteria express specific immunity proteins, called SpaI and NisI. In addition, ABC transporters SpaFEG and NisFEG prevent lantibiotic toxicity by transporting the respective peptides to the extracellular space. Although the three-dimensional structures of SpaI and NisI have been solved, very little is known about the molecular function of either lipoprotein. Using laser-induced liquid bead ion desorption (LILBID)–mass spectrometry, we show here that subtilin interacts with SpaI monomers. The expression of either SpaI or NisI in a subtilin-nonproducing B. subtilis strain resulted in the respective strain being more resistant against either subtilin or nisin. Furthermore, pore formation provided by subtilin and nisin was prevented specifically upon the expression of either SpaI or NisI. As shown with a nisin-subtilin hybrid molecule, the C-terminal part of subtilin but not any particular lanthionine ring was needed for SpaI-mediated immunity. With respect to growth, SpaI provided less immunity against subtilin than is provided by the ABC transporter SpaFEG. However, SpaI prevented pore formation much more efficiently than SpaFEG. Taken together, our data show the physiological function of SpaI as a fast immune response to protect the cellular membrane.IMPORTANCE The two lantibiotics nisin and subtilin are produced by Lactococcus lactis and Bacillus subtilis, respectively. Both peptides have strong antimicrobial activity against Gram-positive bacteria, and therefore, appropriate protection mechanisms are required for the producing strains. To prevent toxicity of their own lantibiotic, both bacteria express immunity proteins, called SpaI and NisI, and in addition, ABC transporters SpaFEG and NisFEG. Whereas it has been shown that the ABC transporters protect the producing strains by transporting the toxic peptides to the extracellular space, the exact mode of action and the physiological function of the lipoproteins during immunity are still unknown. Understanding the exact role of lantibiotic immunity proteins is of major importance for improving production rates and for the design of newly engineered peptide antibiotics. Here, we show (i) the specificity of each lipoprotein for its own lantibiotic, (ii) the specific physical interaction of subtilin with its lipoprotein SpaI, (iii) the physiological function of SpaI in protecting the cellular membrane, and (iv) the importance of the C-terminal part of subtilin for its interaction with SpaI.
机译:枯草芽孢杆菌和乳酸乳球菌分别产生羊毛硫抗生素枯草蛋白酶和乳链菌肽。为了防止自身羊毛硫抗生素的毒性,两种细菌都表达称为SpaI和NisI的特异性免疫蛋白。此外,ABC转运蛋白SpaFEG和NisFEG通过将各自的肽转运到细胞外空间来预防羊毛硫抗生素的毒性。尽管已经解决了SpaI和NisI的三维结构,但对任一种脂蛋白的分子功能知之甚少。使用激光诱导的液珠离子解吸(LILBID)-质谱,我们在这里显示了枯草杆菌蛋白酶与SpaI单体相互作用。在不产生枯草杆菌的枯草芽孢杆菌菌株中,SpaI或NisI的表达导致相应菌株对枯草杆菌蛋白酶或乳链菌肽的抗性更高。此外,在SpaI或NisI表达时,特异性地防止了枯草杆菌蛋白酶和乳链菌肽提供的孔形成。如乳酸链球菌素-枯草杆菌蛋白酶杂合分子所示,SpaI介导的免疫反应不需要枯草杆菌素的C末端,但不需要任何特定的羊毛硫氨酸环。就生长而言,SpaI提供的抗枯草蛋白酶的免疫力比ABC转运蛋白SpaFEG少。但是,SpaI比SpaFEG更有效地阻止了孔的形成。综上所述,我们的数据显示了SpaI作为保护细胞膜的快速免疫反应的生理功能。重要信息乳酸乳球菌和枯草芽孢杆菌分别产生两种乳酸菌素乳链菌肽和枯草杆菌蛋白酶。两种肽对革兰氏阳性细菌均具有很强的抗菌活性,因此,生产菌株需要适当的保护机制。为防止自身羊毛硫抗生素的毒性,两种细菌均表达称为SpaI和NisI的免疫蛋白,此外还表达ABC转运蛋白SpaFEG和NisFEG。尽管已经显示出ABC转运蛋白通过将毒性肽转运到细胞外空间来保护生产菌株,但是在免疫过程中脂蛋白的确切作用方式和生理功能仍然未知。理解羊毛硫抗生素免疫蛋白的确切作用对于提高生产率和设计新设计的肽抗生素至关重要。在这里,我们显示(i)每个脂蛋白对其自身羊毛硫抗生素的特异性,(ii)枯草杆菌蛋白酶与其脂蛋白SpaI的特定物理相互作用,(iii)SpaI在保护细胞膜中的生理功能,以及(iv)枯草杆菌素的C末端部分与SpaI相互作用的重要性。

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