STATegra, a comprehensive multi-omics dataset of B-cell differentiation in mouse

Tarazona, Sonia; Ferreirós-Vidal, Isabel; Ramirez, Ricardo N.; Schmidt, Andreas; Reijmers, Theo H.; Paul, Veronica von Saint; Marabita, Francesco; Rodríguez-Ubreva, Javier; García-Gómez, Antonio; Carroll, Thomas; Cooper, Lee; Liang, Ziwei; Dharmalingam, Gopuraja; Kloet, Frans van der; Harms, Amy C.; Balzano‐Nogueira, Leandro; Lagani, Vincenzo; Tsamardinos, Ioannis; Lappé, Michael; Maier, Dieter; Westerhuis, Johan A.; Hankemeier, Thomas; Imhof, Axel; Ballestar, Esteban; Mortazavi, A; Merkenschlager, Matthias; Tegnér, Jesper; Conesa, Ana

doi:10.1038/s41597-019-0202-7

Cited by 27 publications

(40 citation statements)

References 59 publications

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“…This analysis provided qualitative and quantitative insights into how much the different data-types (e.g., different omics) and their features were “ coordinated ”. Moreover, the analysis provided useful information for targeting specific omics combinations (2). In the third step, for those combinations of omics characterized as coordinated , NPC analysis allowed increasing the statistical power to identify significant features as we have recently demonstrated (40,41).…”

Section: Resultsmentioning

confidence: 99%

“…Thus, instead of looking at the PCA-derived components of mRNA and miRNA separately, we investigated the existence of components (or factors) shared by both omics (47). Intuitively, while in PCA we projected using the main components per omic (refer to Supplementary Figures 2B, 3A as examples), we next aimed to identify projections where the components are informative for more than one data-type simultaneously (refer to Figures 2A, C).…”

Section: Selected Case Studiesmentioning

confidence: 99%

“…Computational and experimental developments have enabled the profiling of multiple layers of cell regulation: genome, transcriptome, epigenome, chromatin conformation or metabolome, among many others globally known “omics” (1,2). The development of such technologies was driven by the understanding that a single-omic does not provide enough information to allow dissecting biological mechanisms (3,4).…”

Section: Introductionmentioning

confidence: 99%

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STATegra: Multi-omics data integration - A conceptual scheme and a bioinformatics pipeline

Planell

Lagani

Sebastián-León

et al. 2020

Preprint

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Technologies for profiling samples using different omics platforms have been at the forefront since the human genome project. Large-scale multi-omics data hold the promise of deciphering different regulatory layers. Yet, while there is a myriad of bioinformatics tools, each multi-omics analysis appears to start from scratch with an arbitrary decision over which tools to use and how to combine them. It is therefore an unmet need to conceptualize how to integrate such data and to implement and validate pipelines in different cases. We have designed a conceptual framework (STATegra), aiming it to be as generic as possible for multi-omics analysis, combining machine learning component analysis, non-parametric data combination and a multi-omics exploratory analysis in a step-wise manner. While in several studies we have previously combined those integrative tools, here we provide a systematic description of the STATegra framework and its validation using two TCGA case studies. For both, the Glioblastoma and the Skin Cutaneous Melanoma cases, we demonstrate an enhanced capacity to identify features in comparison to single-omics analysis. Such an integrative multi-omics analysis framework for the identification of features and components facilitates the discovery of new biology. Finally, we provide several options for applying the STATegra framework when parametric assumptions are fulfilled, and for the case when not all the samples are profiled for all omics. The STATegra framework is built using several tools, which are being integrated step-by-step as OpenSource in the STATegRa Bioconductor package https://bioconductor.org/packages/release/bioc/html/STATegra.html.

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Section: Resultsmentioning

confidence: 99%

Section: Selected Case Studiesmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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STATegra: Multi-omics data integration - A conceptual scheme and a bioinformatics pipeline

Planell

Lagani

Sebastián-León

et al. 2020

Preprint

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“…Cells are renormalized by library count and scaled to unit variance and zero mean. VIA identifies the terminal state at 18-24 h and accurately recapitulates the gene expression trends 26 along inferred pseudotime of IgII1 , Slc7a5 , Fox01 , Myc , Ldha and Lig4 . ( Supplementary Fig.…”

Section: Biological Datamentioning

confidence: 98%

VIA: Generalized and scalable trajectory inference in single-cell omics data

Stassen

Yip

et al. 2021

Preprint

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Inferring cellular trajectories using a variety of omic data is a critical task in single-cell data science. However, prediction and thus biologically meaningful discovery of cell fates are challenged by the sheer size of single-cell data, diverse omic data types, and their complex data topologies. We present VIA, a scalable trajectory inference algorithm that uses lazy-teleporting random walks to accurately reconstruct complex cellular trajectories beyond tree-like pathways (e.g. cyclic or disconnected structures), and to discover less populous lineages or those otherwise obscured in other methods. VIA outperforms existing algorithms in recapitulating cell fates/lineages, and also mitigates loss of global connectivity information in large datasets beyond a million cells. Furthermore, VIA demonstrates versatility by distilling cellular trajectories in single-cell transcriptomic, epigenomic, proteomic and morphological data, showing new promise in scalable, multifaceted single-cell analysis to explore novel biological processes.

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“…Here, we have adopted a multi-omic approach to investigate the set of molecular and cellular events that are associated with MHE. Multi-omic technologies such as genomics, epigenomics, transcriptomics, proteomics and metabolomics are increasingly being used to profile the multi-layered component of living cells and pathological processes 9 – 12 . The rationale behind this strategy is that disease usually impacts different types of biomolecules and by expanding the molecular space under study, the likelihood of identifying relevant biomarkers will increase.…”

Section: Introductionmentioning

confidence: 99%

Multi-omic analysis unveils biological pathways in peripheral immune system associated to minimal hepatic encephalopathy appearance in cirrhotic patients

Rubio

Felipo

Tarazona

et al. 2021

Sci Rep

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Patients with liver cirrhosis may develop minimal hepatic encephalopathy (MHE) which affects their quality of life and life span. It has been proposed that a shift in peripheral inflammation triggers the appearance of MHE. However, the mechanisms involved in this immune system shift remain unknown. In this work we studied the broad molecular changes involved in the induction of MHE with the goal of identifying (1) altered genes and pathways in peripheral blood cells associated to the appearance of MHE, (2) serum metabolites and cytokines with modified levels in MHE patients and (3) MHE-regulated immune response processes related to changes in specific serum molecules. We adopted a multi-omic approach to profile the transcriptome, metabolome and a panel of cytokines of blood samples taken from cirrhotic patients with or without MHE. Transcriptomic analysis supports the hypothesis of alternations in the Th1/Th2 and Th17 lymphocytes cell populations as major drivers of MHE. Cluster analysis of serum molecules resulted in six groups of chemically similar compounds, suggesting that functional modules operate during the induction of MHE. Finally, the multi-omic integrative analysis suggested a relationship between cytokines CCL20, CX3CL1, CXCL13, IL-15, IL-22 and IL-6 with alteration in chemotaxis, as well as a link between long-chain unsaturated phospholipids and the increased fatty acid transport and prostaglandin production. We found altered immune pathways that may collectively contribute to the mild cognitive impairment phenotype in MHE. Our approach is able to combine extracellular and intracellular information, opening new insights to the understanding of the disease.

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STATegra, a comprehensive multi-omics dataset of B-cell differentiation in mouse

Cited by 27 publications

References 59 publications

STATegra: Multi-omics data integration - A conceptual scheme and a bioinformatics pipeline

STATegra: Multi-omics data integration - A conceptual scheme and a bioinformatics pipeline

VIA: Generalized and scalable trajectory inference in single-cell omics data

Multi-omic analysis unveils biological pathways in peripheral immune system associated to minimal hepatic encephalopathy appearance in cirrhotic patients

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