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Integrating large-scale single-cell RNA sequencing in central nervous system disease using self-supervised contrastive learning. | LitMetric

AI Article Synopsis

  • * This study introduces a new method called scCM, which utilizes self-supervised contrastive learning to effectively group similar cells based on gene expression while separating dissimilar ones, allowing for better understanding of the relationships among CNS cell types.
  • * Evaluated across 20 CNS datasets from 4 species and 10 diseases, scCM successfully creates a comprehensive reference for annotating cell types and offers valuable insights into the cellular mechanisms involved in CNS functions and disorders.

Article Abstract

The central nervous system (CNS) comprises a diverse range of brain cell types with distinct functions and gene expression profiles. Although single-cell RNA sequencing (scRNA-seq) provides new insights into the brain cell atlases, integrating large-scale CNS scRNA-seq data still encounters challenges due to the complexity and heterogeneity among CNS cell types/subtypes. In this study, we introduce a self-supervised contrastive learning method, called scCM, for integrating large-scale CNS scRNA-seq data. scCM brings functionally related cells close together while simultaneously pushing apart dissimilar cells by comparing the variations of gene expression, effectively revealing the heterogeneous relationships within the CNS cell types/subtypes. The effectiveness of scCM is evaluated on 20 CNS datasets covering 4 species and 10 CNS diseases. Leveraging these strengths, we successfully integrate the collected human CNS datasets into a large-scale reference to annotate cell types and subtypes in neural tissues. Results demonstrate that scCM provides an accurate annotation, along with rich spatial information of cell state. In summary, scCM is a robust and promising method for integrating large-scale CNS scRNA-seq data, enabling researchers to gain insights into the cellular and molecular mechanisms underlying CNS functions and diseases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11383967PMC
http://dx.doi.org/10.1038/s42003-024-06813-2DOI Listing

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