Multicellular factor analysis of single-cell data for a tissue-centric understanding of disease

Flores, Ricardo O. Ramirez; Lanzer, Jan D.; Dimitrov, Daniel; Velten, Britta; Sáez-Rodríguez, Julio

doi:10.1101/2023.02.23.529642

Cited by 7 publications

(20 citation statements)

References 38 publications

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“…MOFAcellulaR 16 allows the integration of measurements of independent single-cell, spatial, and bulk datasets to contextualize multicellular responses in disease. Inspired by the aforementioned methods, especially MOFAcellulaR 16 , we reutilized MOFA framework in scPAFA for multicellular integration.…”

Section: Discussionmentioning

confidence: 99%

“…A typical primary step in the analysis of scRNA-seq data is to partition the cells into clusters and annotate as cell types 15 ; therefore, downstream analysis commonly focuses on cell-type-centric pairwise cross-condition comparisons, disregarding the multicellular nature of disease processes 16 .…”

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confidence: 99%

“…Gaining advantages from the high flexibility of statistical framework, MOFA was widely applied in different biological contexts, for instance, revealing an axis of heterogeneity associated with the disease outcome in chronic lymphocytic leukemia 19 ; identification of alterations in Alzheimer's disease 20 ; uncovering genotypic, microbiome, and metabolomic factors associated with adenoma and colorectal cancer risk 21 . Inspired by Ramirez et al 16 , we reutilized MOFA to identify multicellular pathway modules.…”

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confidence: 99%

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Uncovering disease-related multicellular pathway modules on large-scale single-cell transcriptomes with scPAFA

Huang,

Zheng,

Wang

et al. 2024

Preprint

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Pathway analysis is a crucial analytical phase in disease research on single-cell RNA sequencing (scRNA-seq) data, offering biological interpretations based on prior knowledge. However, currently available tools for generating cell-level pathway activity scores (PAS) exhibit computational inefficacy in large-scale scRNA-seq datasets. Besides, disease-related pathways are commonly identified by cross-condition comparisons in each cell type, neglecting the potential multicellular patterns. Here, we present single-cell pathway activity factor analysis (scPAFA), a Python library designed for large-scale single-cell dataset allowing rapid PAS computation and uncovering biologically interpretable disease-related multicellular pathway modules, which are low-dimensional representations of disease-related PAS variance in multiple cell types. Application on colorectal cancer (CRC) dataset with 371,223 cells and large-scale lupus atlas over 1.2 million cells demonstrated that scPAFA can achieve > 33-fold decreases in runtime of PAS computation and further identified reliable and interpretable multicellular pathway modules that capture the transcriptomic features of CRC tumor status and transcriptional abnormalities in lupus patients, respectively.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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confidence: 99%

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Uncovering disease-related multicellular pathway modules on large-scale single-cell transcriptomes with scPAFA

Huang,

Zheng,

Wang

et al. 2024

Preprint

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“…This demonstration that patients with long-standing MS differ markedly in the transcriptional signatures of their glia, whatever their lesion classification, but which fall into apparent subgroups, is important in the context of the variable responses to experimental neuroprotective therapies for example targeting remyelination. To explore these apparent subgroups more, and to understand the underlying cellular and molecular mechanisms, we adapted MOFA+, a computational method originally developed for identifying low-dimensional representations of variation across multiple data modalities 29 to identify similar donor-associated transcriptional patterns across multiple cell types (modalities) simultaneously 29,30 . For each cell type, we selected genes with evidence of a MS effect and/or a donor effect (Extended Data Fig.…”

Section: Coordinated Multicellular Gene Expression Programs Define Pa...mentioning

confidence: 99%

Single nuclei RNAseq stratifies multiple sclerosis patients into distinct white matter glial responses

Macnair

Calini

Agirre

et al. 2022

Preprint

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The lack of understanding as to the cellular and molecular basis of clinical and genetic heterogeneity in progressive multiple sclerosis (MS) has hindered the search for new effective therapies and biomarkers. Here, to address this gap, we analysed 740,000 single nuclei RNAseq profiles of 165 samples of white matter (WM) lesions, normal appearing WM, grey matter (GM) lesions and normal appearing GM from 55 MS patients and 28 controls. We find that gene expression changes in response to MS are highly cell-type specific in WM and GM lesions but are largely shared within an individual cell-type across lesions, following a continuum rather than discrete lesion-specific molecular programs. The major biological determinants of variability in gene expression in MS samples relate to individual patient effects, rather than to lesion types or other metadata. Using multi-omics factor analysis (MOFA+), we identify three subgroups of MS patients with distinct oligodendrocyte composition and WM glial gene expression signatures, suggestive of engagement of different pathological/regenerative processes. The discovery of these three patterns significantly advances our mechanistic understanding of progressive MS, provides a framework to use molecular biomarkers to stratify patients for best therapeutic approaches for progressive MS, and highlights the need for precision-medicine approaches to address heterogeneity among MS patients.

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“…Moreover, most tools do not account for the relationships of coordinated CCC events (CCC programs) across different contexts 4 , either disregarding context altogether by analyzing samples individually or being limited to pairwise comparisons. Thus, as the ability to generate large single-cell and spatial transcriptomics datasets and the interest in studying CCC programs continues to increase [5][6][7] , the need to robustly decipher CCC is becoming essential.…”

Section: Introductionmentioning

confidence: 99%

Combining LIANA and Tensor-cell2cell to decipher cell-cell communication across multiple samples

Baghdassarian

Dimitrov

Armingol

et al. 2023

Preprint

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In recent years, data-driven inference of cell-cell communication has helped reveal coordinated biological processes across cell types. While multiple cell-cell communication tools exist, results are specific to the tool of choice, due to the diverse assumptions made across computational frameworks. Moreover, tools are often limited to analyzing single samples or to performing pairwise comparisons. As experimental design complexity and sample numbers continue to increase in single-cell datasets, so does the need for generalizable methods to decipher cell-cell communication in such scenarios. Here, we integrate two tools, LIANA and Tensor-cell2cell, which combined can deploy multiple existing methods and resources, to enable the robust and flexible identification of cell-cell communication programs across multiple samples. In this protocol, we show how the integration of our tools facilitates the choice of method to infer cell-cell communication and subsequently perform an unsupervised deconvolution to obtain and summarize biological insights. We explain how to perform the analysis step-by-step in both Python and R, and we provide online tutorials with detailed instructions available at https://ccc-protocols.readthedocs.io/. This protocol typically takes ~1.5h to complete from installation to downstream visualizations on a GPU-enabled computer, for a dataset of ~63k cells, 10 cell types, and 12 samples.

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Multicellular factor analysis of single-cell data for a tissue-centric understanding of disease

Cited by 7 publications

References 38 publications

Uncovering disease-related multicellular pathway modules on large-scale single-cell transcriptomes with scPAFA

Uncovering disease-related multicellular pathway modules on large-scale single-cell transcriptomes with scPAFA

Single nuclei RNAseq stratifies multiple sclerosis patients into distinct white matter glial responses

Combining LIANA and Tensor-cell2cell to decipher cell-cell communication across multiple samples

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