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Transitioning from nanoflow to standard flow LC/MS: High throughput protein biomarker quantification for clinical research

RECORD | Already taken place Th, 28.1.2021
This webinar will discuss the analytical performance under standard-flow and low LC flow conditions using the Agilent 6495 triple quadrupole LC/MS system.
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Agilent Technologies: Transitioning from nanoflow to standard flow LC/MS: High throughput protein biomarker quantification for clinical research
Agilent Technologies: Transitioning from nanoflow to standard flow LC/MS: High throughput protein biomarker quantification for clinical research

Liquid chromatography-mass spectrometry-based proteomics has been widely used for protein biomarker discovery and validation. When transitioning from discovery proteomics to targeted protein biomarker quantification, the MRM-based LC/MS method plays an important role in clinical research. To ensure analytical reproducibility and robustness, implementing a standard flow-based triple quadrupole LC/MS system has a tremendous benefit when involving a large cohort.

Learning Objectives:

  • Quantitative sensitivity, precision, and accuracy of standard flow-based dynamic MRM method for targeted protein biomarker analysis using the Agilent 6495 LC/TQ
  • Successful transfer of PromarkerD method for diabetic kidney disease research from nanoflow to standard flow
  • When sample limited, a low flow LC system, Evosep One, coupled to Agilent 6495 LC/TQ could be used for high throughput studies

For Research Use Only. Not for use in diagnostic procedures.

Presenter: Linfeng Wu, Ph.D. (LC/MS Application Scientist, Agilent Technologies)

Dr. Linfeng Wu received her Ph.D. in 2007 at University of Connecticut for Biomedical Sciences. After a postdoctoral training in Dr. Michael Snyder’s group at Stanford University, she worked as a research scientist in biotech industry focusing on protein biomarker discovery and multi-omics integration in personalized medicine. Dr. Wu joined Agilent in 2015 as an application scientist, focusing on LC/MS-based protein, proteomics and small molecule analyses.

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