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巯基衍生化用于复杂基质中微囊藻毒素的 LC-MS 鉴定。

Thiol derivatization for LC-MS identification of microcystins in complex matrices.

机构信息

Norwegian Veterinary Institute, P.O. Box 750 Sentrum, 0106 Oslo, Norway.

出版信息

Environ Sci Technol. 2012 Aug 21;46(16):8937-44. doi: 10.1021/es301808h. Epub 2012 Aug 10.

Abstract

Microcystins are a group of cyclic heptapeptides originating from cyanobacteria. Cyanobacteria also produce a range of peptides and other compounds that can result in complex chromatograms when samples are analyzed by LC-MS. Derivatization with appropriate thiols (e.g., mercaptoethanol) of the olefin in the α,β-unsaturated amide present in most microcystins was shown to simplify analysis of LC-MS chromatograms of sample extracts, making it much easier to identify peaks corresponding to candidate microcystins. Furthermore, interpretation of MS(2) spectra was facilitated by addition of the mass associated with the thiol to the α,β-unsaturated amide of microcystins. Cyanotoxins containing Mdha or Dha reacted readily with thiols, whereas Mser, Ser, Mdhb, and thiol-derivatives of Mdha or Dha did not react under the conditions used. This approach therefore provides a convenient LC-MS method to obtain evidence for the presence of Mdha or Dha and can likely be used to differentiate between the isobaric amino acids Mdha and Dhb in candidate cyanotoxin peaks. When O-(2-mercaptoethyl)-O'-methyl-hexa(ethylene glycol) (MEMHEG) (M(w)t. 356) was used as the thiol, the resulting derivatives eluted in an LC-MS mass window that was largely free of interferences. This approach simplifies detection of candidate microcystin analogues even in the presence of complex mixtures of coeluting components. The method was used for qualitative analysis of a Microcystis aeruginosa culture from Lake Naivasha, Kenya, and the results were verified using precursor-ion scanning and high-resolution mass spectrometry.

摘要

微囊藻毒素是一组来源于蓝藻的环七肽。蓝藻还会产生一系列肽和其他化合物,当用 LC-MS 对样品进行分析时,这些化合物会导致复杂的色谱图。用适当的硫醇(例如巯基乙醇)对大多数微囊藻毒素中存在的α,β-不饱和酰胺中的烯烃进行衍生化,简化了 LC-MS 色谱图中样品提取物的分析,使得更容易识别对应候选微囊藻毒素的峰。此外,通过将与硫醇相关的质量添加到微囊藻毒素的α,β-不饱和酰胺中,有助于解释 MS(2)谱。含有 Mdha 或 Dha 的蓝藻毒素很容易与硫醇反应,而 Mser、Ser、Mdhb 以及 Mdha 或 Dha 的硫醇衍生物在使用的条件下没有反应。因此,该方法提供了一种方便的 LC-MS 方法,可以获得存在 Mdha 或 Dha 的证据,并且可能可用于区分候选蓝藻毒素峰中同量异位的氨基酸 Mdha 和 Dhb。当使用 O-(2-巯基乙基)-O'-甲基-六(乙二醇)(MEMHEG)(分子量 356)作为硫醇时,得到的衍生物在 LC-MS 质量窗口中洗脱,该窗口基本没有干扰。即使在复杂的共洗脱成分混合物存在的情况下,该方法也简化了候选微囊藻毒素类似物的检测。该方法用于定性分析肯尼亚奈瓦沙湖的铜绿微囊藻培养物,结果使用前体离子扫描和高分辨率质谱进行验证。

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