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规避产品毒性影响:开发一种用于羊毛硫抗生素加利杀菌素的新型两阶段生产工艺。

Circumventing the effect of product toxicity: development of a novel two-stage production process for the lantibiotic gallidermin.

作者信息

Valsesia G, Medaglia G, Held M, Minas W, Panke S

机构信息

Bioprocess Laboratory, Institute for Process Engineering, ETH Zentrum CNB E122.1, Universitätstr. 6, 8092 Zürich, Switzerland.

出版信息

Appl Environ Microbiol. 2007 Mar;73(5):1635-45. doi: 10.1128/AEM.01969-06. Epub 2006 Dec 28.

Abstract

Lantibiotics such as gallidermin are lanthionine-containing polypeptide antibiotics produced by gram-positive bacteria that might become relevant for the treatment of various infectious diseases. So far, self-toxicity has prevented the isolation of efficient overproducing strains, thus hampering their thorough investigation and preventing their exploitation in fields other than the food area. We wanted to investigate the effect of lantibiotic precursor peptides on the producing strains in order to evaluate novel strategies for the overproduction of these promising peptides. In this study, gallidermin was chosen as a representative example of the type A lantibiotics. A Staphylococcus gallinarum Tü3928 mutant, whose gene for the extracellular pregallidermin protease GdmP was replaced by a kanamycin-resistance gene, was constructed. Mass spectrometry (MS) analysis indicated that this mutant produced fully posttranslationally modified gallidermin precursors with truncated versions of the leader peptide, but not the entire leader as predicted from the gdmA sequence. In filter-on-plate assays, these truncated pregallidermins showed no toxicity against Staphylococcus gallinarum Tü3928 up to a concentration of 8 g/liter (corresponding to approximately 2.35 mM), while gallidermin produced clear inhibitory zones at concentrations as low as 0.25 g/liter (0.12 mM). We showed that the lack of toxicity is due entirely to the presence of the truncated leader, since MS as well as bioassay analysis showed that the peptides resulting from tryptic cleavage of pregallidermins and gallidermin produced by S. gallinarum Tü3928 had identical masses and approximately the same specific activity. This demonstrates that even a shortened leader sequence is sufficient to prevent the toxicity of mature gallidermin. In nonoptimized fermentations, the gdmP mutant produced pregallidermin to a 50%-higher molar titer, suggesting that the absence of self-toxicity has a beneficial effect on gallidermin production and giving a first confirmation of the suitability of the overproduction strategy.

摘要

诸如加里德明之类的羊毛硫抗生素是由革兰氏阳性菌产生的含羊毛硫氨酸的多肽抗生素,可能与各种传染病的治疗相关。到目前为止,自身毒性阻碍了高效过量生产菌株的分离,从而妨碍了对它们的深入研究,并阻止了它们在食品领域以外的其他领域的应用。我们想要研究羊毛硫抗生素前体肽对生产菌株的影响,以便评估这些有前景的肽过量生产的新策略。在本研究中,加里德明被选为A型羊毛硫抗生素的代表性例子。构建了一株鸡葡萄球菌Tü3928突变体,其细胞外前加里德明蛋白酶GdmP的基因被卡那霉素抗性基因取代。质谱(MS)分析表明,该突变体产生了翻译后完全修饰的加里德明前体,其前导肽为截短形式,而不是gdmA序列预测的完整前导肽。在滤膜平板试验中,这些截短的前加里德明在浓度高达8 g/升(约相当于2.35 mM)时对鸡葡萄球菌Tü3928没有毒性,而加里德明在低至0.25 g/升(0.12 mM)的浓度下就产生了明显的抑制圈。我们表明,缺乏毒性完全是由于截短的前导肽的存在,因为MS以及生物测定分析表明,鸡葡萄球菌Tü3928产生的前加里德明和加里德明经胰蛋白酶切割产生的肽具有相同的质量和大致相同的比活性。这表明,即使是缩短的前导序列也足以防止成熟加里德明的毒性。在未优化的发酵中,gdmP突变体产生前加里德明的摩尔滴度提高了50%,这表明缺乏自身毒性对加里德明的生产有有益影响,并首次证实了过量生产策略的适用性。

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