Abstract

Lipid quantification is the ultimate goal in lipidomics studies challenged by the availability of standard compounds. A novel strategy for targeted lipidomics based on LC-MS/MS parameters prediction and multivariate statistical analysis was developed for the quantitation of lysophosphatidylcholines (LPCs) in this study. Multiple linear regression models were established with the acyl chain length and number of double bonds after the prediction correlation coefficients ( R2pred) were evaluated. Then related analytical parameters including collision energy, declustering potential, retention time, and response factor were successfully predicted for any given LPC. With this "model-prediction" strategy, sensitivity, accuracy, and coverage of targeted lipidomics were improved significantly, and 60 LPCs were determined simultaneously in plasma for the first time. An integrated evaluation method for multi-indexes, logistic regression-ROC analysis was also proposed after biomarkers were identified by Student's t test, univariate ROC curve, and PLS-DA. Then the developed workflow was successfully used to discover and evaluate multi-LPCs indexes (a set of LPCs biomarkers with the best discriminating ability) for differentiating lung, breast, colorectal, and gastric cancer from controls, and among different types of cancer. Finally, the multi-LPCs index for lung cancer was compared with the plasma before and after treatment to test its utility. The novel targeted lipidomics methodology for LPCs was expected to provide a new insight into quantitative lipidomics and further clinical application.

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