CLUE-TIPS, clustering methods for pattern analysis of LC-MS data

Abstract

Liquid Chromatography Mass Spectrometry (LC-MS) based proteomics is an important tool in detecting changes in peptide/protein abundances in samples potentially leading to the discovery of disease biomarker candidates. We present CLUE-TIPS (Clustering Using Euclidean distance in Tanimoto Inter-Point Space), an approach that compares complex proteomic samples for similarity/dissimilarity analysis. In CLUE-TIPS, an intersample distance feature map is generated from filtered, aligned and binarized raw LC-MS data by applying the Tanimoto distance metric to obtain normalized similarity scores between all sample pairs for each m/z value. We developed clustering and visualization methods for the intersample distance map to analyze various samples for differences at the sample level as well as the individual m/z level. An approach to query for specific m/z values that are associated with similarity/dissimilarity patterns in a set of samples was also briefly described. CLUE-TIPS can also be used as a tool in assessing the quality of LC-MS runs. The presented approach does not rely on tandem mass-spectrometry (MS/MS), isotopic labels or gels and also does not rely on feature extraction methods. CLUE-TIPS suite was applied to LC-MS data obtained from plasma samples collected at various time points and treatment conditions from immunosuppressed mice implanted with MCF-7 human breast cancer cells. The generated raw LC-MS data was used for pattern analysis and similarity/dissimilarity detection. CLUE-TIPS successfully detected the differences/similarities in samples at various time points taken during the progression of tumor, and also recognized differences/similarities in samples representing various treatment conditions.