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首页> 外文期刊>Biomedical Chromatography: An International Journal Devoted to Research in Chromatographic Methodologies and Their Applications in the Biosciences >Switching from an analogous to a stable isotopically labeled internal standard for the LC-MS/MS quantitation of the novel anticancer drug Kahalalide F significantly improves assay performance.
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Switching from an analogous to a stable isotopically labeled internal standard for the LC-MS/MS quantitation of the novel anticancer drug Kahalalide F significantly improves assay performance.

机译:从LC-MS / MS定量的新型抗癌药物Kahalalide F的类似同位素标记内标转换为稳定同位素内标,显着提高了测定性能。

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摘要

The importance of a stable isotopically labeled (SIL) internal standard for the quantitative LC-MS/MS assay for Kahalalide F in human plasma is highlighted. Similar results can be expected for other LC-MS/MS assays. Therefore, we emphasize the need for an SIL internal standard for accurate and precise LC-MS/MS assays of drugs in biological matrices.
机译:强调了稳定的同位素标记(SIL)内标对于人血浆中Kahalalide F的定量LC-MS / MS测定的重要性。对于其他LC-MS / MS分析,也有望获得类似的结果。因此,我们强调需要使用SIL内标来对生物基质中的药物进行准确而精确的LC-MS / MS分析。

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