Targeted realignment of LC-MS profiles by neighbor-wise compound-specific graphical time warping with misalignment detection

Chao, Wu; Wang, Yizhi; Wang, Yinxue; Ebbels, Timothy M. D.; Karaman, Íbrahím; Graça, Gonçalo; Pinto, Rui; Herrington, David M.; Wang, Yue; Yu, Guoqiang

doi:10.1093/bioinformatics/btaa037

Cited by 14 publications

(9 citation statements)

References 25 publications

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“…Due to hardware limitations, individual batches of both experiments are treated as distinct tables prior to their alignment with metabCombiner . While it is possible to simultaneously align LC-MS metabolomics batches of the same experiment using conventional open-source preprocessing tools, such as XCMS, this has some disadvantages, such as a tendency to misalign features in large-scale experiments due to excess chromatographic drift , and generation of false positive features due to peak detection inaccuracies . The application of our methods reduced the feature lists to a common intersection of compounds found across all experimental batches, facilitating a well-powered statistical analysis.…”

Section: Discussionmentioning

confidence: 99%

Alignment and Analysis of a Disparately Acquired Multibatch Metabolomics Study of Maternal Pregnancy Samples

et al. 2022

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Untargeted liquid chromatography−mass spectrometry metabolomics studies are typically performed under roughly identical experimental settings. Measurements acquired with different LC-MS protocols or following extended time intervals harbor significant variation in retention times and spectral abundances due to altered chromatographic, spectrometric, and other factors, raising many data analysis challenges. We developed a computational workflow for merging and harmonizing metabolomics data acquired under disparate LC-MS conditions. Plasma metabolite profiles were collected from two sets of maternal subjects three years apart using distinct instruments and LC-MS procedures. Metabolomics features were aligned using metabCombiner to generate lists of compounds detected across all experimental batches. We applied data set-specific normalization methods to remove interbatch and interexperimental variation in spectral intensities, enabling statistical analysis on the assembled data matrix. Bioinformatics analyses revealed large-scale metabolic changes in maternal plasma between the first and third trimesters of pregnancy and between maternal plasma and umbilical cord blood. We observed increases in steroid hormones and free fatty acids from the first trimester to term of gestation, along with decreases in amino acids coupled to increased levels in cord blood. This work demonstrates the viability of integrating nonidentically acquired LC-MS metabolomics data and its utility in unconventional metabolomics study designs.

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Section: Discussionmentioning

confidence: 99%

Alignment and Analysis of a Disparately Acquired Multibatch Metabolomics Study of Maternal Pregnancy Samples

et al. 2022

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“…neighbor-wise compound-specific Graphical Time Warping (ncGTW) , is an integrated reference-free profile alignment method, implemented as an R-package and is available as a plugin for xcms that aids in detecting and fixing the bad alignments (misaligned feature groups) in the LC–MS data to render accurate grouping and peak-filling (Wu et al 2020 ).…”

Section: Preprocessing and Quality Control (Qc) Toolsmentioning

confidence: 99%

New software tools, databases, and resources in metabolomics: updates from 2020

Misra

2021

Metabolomics

149

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Background Precision medicine, space exploration, drug discovery to characterization of dark chemical space of habitats and organisms, metabolomics takes a centre stage in providing answers to diverse biological, biomedical, and environmental questions. With technological advances in mass-spectrometry and spectroscopy platforms that aid in generation of information rich datasets that are complex big-data, data analytics tend to co-evolve to match the pace of analytical instrumentation. Software tools, resources, databases, and solutions help in harnessing the concealed information in the generated data for eventual translational success. Aim of the review In this review, ~ 85 metabolomics software resources, packages, tools, databases, and other utilities that appeared in 2020 are introduced to the research community. Key scientific concepts of review In Table 1 the computational dependencies and downloadable links of the tools are provided, and the resources are categorized based on their utility. The review aims to keep the community of metabolomics researchers updated with all the resources developed in 2020 at a collated avenue, in line with efforts form 2015 onwards to help them find these at one place for further referencing and use.

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“…Our approach also corrects raw files prior to peak detection and alignment but does not require heavy isotope labelled standards. Another study in which alignment between samples from a large-scale dataset (N = 1000) is addressed [30] proposed a profile-based alignment algorithm which uses a graphical time warping method to correct the retention times for mis-aligned features.…”

Section: Alignment Of Disparate Lc-ms Datasetsmentioning

confidence: 99%

Alignment of multiple metabolomics LC-MS datasets from disparate diseases to reveal fever-associated metabolites

Năstase

Barrett

Cárdenas

et al. 2021

Preprint

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Acute febrile illnesses are still a major cause of mortality and morbidity globally, particularly in low to middle income countries. The aim of this study was to determine any possible metabolic commonalities of patients infected with disparate pathogens that cause fever. Three liquid chromatography-mass spectrometry (LC-MS) datasets investigating the metabolic effects of malaria, leishmaniasis and Zika virus infection were used. The retention time (RT) drift between the datasets was determined using landmarks obtained from the standard reference mixtures generally used in the quality control of the LC-MS experiments. We used fitted Gaussian Process models (GPs) to perform a high level correction of the RT drift between the experiments, followed by standard peakset alignment between the samples with corrected RTs of the three LC-MS datasets. Statistical analysis, annotation and pathway analysis of the integrated peaksets were subsequently performed. Metabolic dysregulation patterns common across the datasets were identified, with kynurenine pathway being the most affected pathway between all three fever-associated datasets.

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Targeted realignment of LC-MS profiles by neighbor-wise compound-specific graphical time warping with misalignment detection

Cited by 14 publications

References 25 publications

Alignment and Analysis of a Disparately Acquired Multibatch Metabolomics Study of Maternal Pregnancy Samples

Alignment and Analysis of a Disparately Acquired Multibatch Metabolomics Study of Maternal Pregnancy Samples

New software tools, databases, and resources in metabolomics: updates from 2020

Alignment of multiple metabolomics LC-MS datasets from disparate diseases to reveal fever-associated metabolites

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