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A highly sensitive and selective high pressure liquid chromatography with tandem mass spectrometry (HPLC/MS-MS) method for the direct peptide reactivity assay (DPRA)

机译:具有串联质谱(HPLC / MS-MS)的高敏感和选择性的高压液相色谱法,用于直接肽反应性测定法(DPRA)

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摘要

While the HPLC/UV (high performance liquid chromatography coupled with ultra-violet spectrometry)-based DPRA (Direct Peptide Reactivity Assay) identifies dermal sensitizers with approximately 80% accuracy, the low selectivity and sensitivity of the HPLC/UV-based DPRA poses challenges to accurately identify the sensitization potential of certain chemicals. In this study, a high performance liquid chromatography coupled with tandem mass spectrometry (HPLC/MS-MS)-based DPRA was developed and validated according to the test guideline (OECD TG 442C). The final results were compared with the results from the traditional HPLC/UV-based guideline DPRA. This HPLC/MS-MS-based DPRA demonstrated similar performance compared to HPLC/UV-based DPRA using known dermal sensitizers and non-sensitizers according to the test guideline (OECD TG 442C). Following the validation, a challenge set of chemicals with either overlapping retention time with peptides, or higher hydrophobicity or chemicals potentially forming non-covalent interactions with peptides were assessed for dermal sensitization potential using both methods and the results were compared to existing in vivo data. The HPLC/MS-MS-based DPRA correctly predicted these chemicals as sensitizers or non-sensitizers; however, the HPLC/UV-based DPRA resulted in false-positive predictions for hydrophobic substances, chemicals with UV peaks overlapping with those of the peptide(s), and compounds that non-covalently interact with the peptides. These findings demonstrate the broader applicability and better sensitivity and selectivity of the LC/MS-MS-based DPRA over the traditional HPLC/UV-based guideline DPRA.
机译:虽然HPLC / UV(高性能液相色谱与紫外光谱谱偶联)基于DPRA(直接肽反应性测定)鉴定了大约80%的精度,但HPLC / UV的DPRA的低选择性和敏感性呈现了大约80%的皮肤敏化剂准确识别某些化学品的敏化潜力。在该研究中,根据试验准则(OECD TG 442C)开发并验证了与串联质谱(HPLC / MS-MS)偶联的高效液相色谱法。将最终结果与来自基于传统的HPLC / UV的指南DPRA的结果进行比较。基于HPLC / MS-MS的DPRA与使用已知的真皮敏化剂和非敏化剂的基于HPLC / UV的DPRA相比,根据测试指南(OECD TG 442C)相比,与基于HPLC / UV的DPRA相比,表现出类似的性能。在验证之后,评估使用两种方法的肽与肽的重叠保留时间与肽的重叠保留时间或潜在地形成非共价相互作用的较高疏水性或化学物质进行挑战,或者潜在地形成与肽的非共价相互作用。基于HPLC / MS-MS的DPRA正确预测这些化学品作为敏感剂或非敏化剂;然而,基于HPLC / UV的DPRA导致疏水性物质的假阳性预测,与肽重叠的UV峰值的化学品,以及非共价相互作用的化合物与肽相互作用。这些发现表明,通过传统的HPLC / UV的指南DPRA,展示了更广泛的适用性和基于LC / MS-MS-MS的DPRA的更好的敏感性和选择性。

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    Dow Chem Co USA Toxicol &

    Environm Res &

    Consulting 1803 Bldg Midland MI 48674 USA;

    Dow Chem Co USA Toxicol &

    Environm Res &

    Consulting 1803 Bldg Midland MI 48674 USA;

    Dow Chem Co USA Toxicol &

    Environm Res &

    Consulting 1803 Bldg Midland MI 48674 USA;

    Dow Chem Co USA Toxicol &

    Environm Res &

    Consulting 1803 Bldg Midland MI 48674 USA;

    Dow Chem Co USA Toxicol &

    Environm Res &

    Consulting 1803 Bldg Midland MI 48674 USA;

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  • 正文语种 eng
  • 中图分类 药理学;
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