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利用基质辅助激光解吸电离飞行时间质谱法对多粘芽孢杆菌-M1产生的新型杀镰孢菌素进行表征

Characterization of Novel Fusaricidins Produced by Paenibacillus polymyxa-M1 Using MALDI-TOF Mass Spectrometry.

作者信息

Vater Joachim, Niu Ben, Dietel Kristin, Borriss Rainer

机构信息

Institut für Chemie, Technische Universität Berlin, Mueller-Breslau-Straße 10, 10623, Berlin, Germany,

出版信息

J Am Soc Mass Spectrom. 2015 Sep;26(9):1548-58. doi: 10.1007/s13361-015-1130-1. Epub 2015 Jun 23.

Abstract

Paenibacillus polymyxa-M1 is a potent producer of bioactive compounds, such as lipopeptides, polyketides, and lantibiotics of biotechnological and medical interest. Genome sequencing revealed nine gene clusters for nonribosomal biosynthesis of such agents. Here we report on the investigation of the fusaricidins, a complex of cyclic lipopeptides containing 15-guanidino-3-hydroxypentadecanoic acid (GHPD) as fatty acid component by matrix-assisted laser-desorption/ionization time-of-flight mass spectrometry (MALDI-TOF MS). More than 20 variants of these compounds were detected and characterized in detail. Mass spectrometric sequence analysis was performed by MALDI-LIFT-TOF/TOF fragment analysis. The obtained product ion spectra show a specific processing in the fatty acid part. GHPD is cleaved between the α- and ß-position yielding two fragments a and b, one bearing the end-standing guanidine group and another one comprising the residual two C-atoms of GHPD with the attached peptide moiety. The complete sequence of all fusaricidins was derived from sets of bn- and yn-ions. The fusaricidin complex can be divided into four lipopeptide families, three of them showing variations of the amino acid in position 3, Val or Ile for the first and Tyr or Phe for families 2 and 3, respectively. A collection of novel fusaricidins was detected differing from those of families 1-3 by an additional residue of 71 Da (family 4). LIFT-TOF/TOF fragment spectra of these species imply that in their peptide moiety, an Ala-residue is attached by an ester bond to the free hydroxyl group of Thr4. More than 10 novel fusaricidins were characterized mass spectrometrically.

摘要

多粘类芽孢杆菌-M1是生物活性化合物的高效生产者,这些生物活性化合物包括具有生物技术和医学价值的脂肽、聚酮化合物和羊毛硫抗生素。基因组测序揭示了九个用于此类物质非核糖体生物合成的基因簇。在此,我们报告了通过基质辅助激光解吸/电离飞行时间质谱(MALDI-TOF MS)对fusaricidins(一种含有15-胍基-3-羟基十五烷酸(GHPD)作为脂肪酸成分的环脂肽复合物)的研究。检测到这些化合物的20多种变体并对其进行了详细表征。通过MALDI-LIFT-TOF/TOF片段分析进行质谱序列分析。所得产物离子光谱显示了脂肪酸部分的特定加工过程。GHPD在α和β位之间裂解,产生两个片段a和b,一个带有末端胍基,另一个包含带有连接肽部分的GHPD的剩余两个碳原子。所有fusaricidins的完整序列来自bn-和yn-离子组。fusaricidin复合物可分为四个脂肽家族,其中三个家族在第3位氨基酸上存在变异,第一个家族为Val或Ile,第2和第3家族分别为Tyr或Phe。检测到一组新型fusaricidins,它们与第1-3家族的fusaricidins不同,有一个额外的71 Da残基(第4家族)。这些物种的LIFT-TOF/TOF片段光谱表明,在其肽部分,一个Ala残基通过酯键连接到Thr4的游离羟基上。通过质谱对10多种新型fusaricidins进行了表征。

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