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高通量液质联用技术/质谱法,采用精确质量技术对小分子物质进行定量分析,支持药物筛选的发现。

High-throughput liquid chromatography/mass spectrometry method for the quantitation of small molecules using accurate mass technologies in supporting discovery drug screening.

机构信息

Genentech, Inc., Drug Metabolism and Pharmacokinetics, MS 412A, 1 DNA Way, South San Francisco, CA 94080, USA.

出版信息

Rapid Commun Mass Spectrom. 2013 Feb 15;27(3):401-8. doi: 10.1002/rcm.6461.

Abstract

RATIONALE

Drug discovery samples are routinely analyzed using liquid chromatography/tandem mass spectrometry (LC/MS/MS) methods on triple quadrupole mass spectrometers employing multiple reaction monitoring (MRM). In order to improve analysis throughput, quantitation of small molecules on a quadrupole time-of-flight (QqTOF) instrument using TOF scan and high-resolution MRM (MRM-HR) modes was evaluated in this study.

METHODS

Cassette dosed plasma and brain samples from nine compounds were extracted using a protein precipitation method. Separation was achieved by reversed-phase liquid chromatography. Mass spectrometric analysis was performed using TOF scan and high-resolution MRM approaches on a QqTOF mass spectrometer with turbo-ionspray ionization. Results were compared to those obtained on a triple quadrupole mass spectrometer.

RESULTS

The dynamic range varied depending on compounds and instruments and was similar between the MRM on QqQ and full TOF scan mode on QqTOF. Linear or quadratic regression and 1/x(2) weighting were used. Resolution on the QqTOF instrument was around 32000 and mass accuracy was within 4.4 ppm. The MRM-HR method showed better sensitivity compared to the TOF scan method, and was comparable to the MRM on a QqQ mass spectrometer. Assay accuracy was within ±25%.

CONCLUSIONS

A TOF scan method allowed the use of the generic method without compound-specific optimization and was an alternative choice for routine high-throughput quantitation of small molecules. The MRM-HR method on the QqTOF showed good sensitivity which was comparable to that obtained by the MRM method on the triple quadrupole mass spectrometer.

摘要

理由

药物发现样品通常使用三重四极杆质谱仪上的液相色谱/串联质谱 (LC/MS/MS) 方法,采用多重反应监测 (MRM) 进行分析。为了提高分析通量,本研究评估了在四极杆飞行时间 (QqTOF) 仪器上使用 TOF 扫描和高分辨率 MRM (MRM-HR) 模式对小分子进行定量的方法。

方法

采用蛋白沉淀法提取 9 种化合物的盒式剂量血浆和脑样品。采用反相液相色谱进行分离。使用涡轮离子喷雾电离的 QqTOF 质谱仪进行质谱分析,采用 TOF 扫描和高分辨率 MRM 方法。结果与三重四极杆质谱仪的结果进行比较。

结果

动态范围取决于化合物和仪器,在 QqQ 上的 MRM 和 QqTOF 上的全 TOF 扫描模式之间相似。使用线性或二次回归和 1/x(2) 加权。QqTOF 仪器的分辨率约为 32000,质量精度在 4.4 ppm 以内。MRM-HR 方法比 TOF 扫描方法具有更好的灵敏度,与 QqQ 质谱仪上的 MRM 相当。测定准确度在±25%以内。

结论

TOF 扫描方法允许使用通用方法而无需对化合物进行特定优化,是常规高通量小分子定量的替代选择。QqTOF 上的 MRM-HR 方法具有良好的灵敏度,与三重四极杆质谱仪上的 MRM 方法相当。

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