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Global coordination level in single-cell transcriptomic data. | LitMetric

AI Article Synopsis

  • - The text discusses the challenge of assessing coordination between genes using single-cell transcriptomic data without prior knowledge of gene regulatory interactions, introducing a 'top-down' approach that evaluates global coordination levels (GCL) among genes.
  • - The study reveals that individual outlier cells can significantly influence the GCL calculations across a group of cells and that the presence of gene clusters, commonly found in scRNA-seq data, also impacts the GCL results.
  • - The research includes an analysis of the Jackknife sampling method's effect on GCL statistics and provides a custom Python package for calculating GCL, offering guidelines for effective pre-processing and interpretation of gene expression data.

Article Abstract

Genes are linked by underlying regulatory mechanisms and by jointly implementing biological functions, working in coordination to apply different tasks in the cells. Assessing the coordination level between genes from single-cell transcriptomic data, without a priori knowledge of the map of gene regulatory interactions, is a challenge. A 'top-down' approach has recently been developed to analyze single-cell transcriptomic data by evaluating the global coordination level between genes (called GCL). Here, we systematically analyze the performance of the GCL in typical scenarios of single-cell RNA sequencing (scRNA-seq) data. We show that an individual anomalous cell can have a disproportionate effect on the GCL calculated over a cohort of cells. In addition, we demonstrate how the GCL is affected by the presence of clusters, which are very common in scRNA-seq data. Finally, we analyze the effect of the sampling size of the Jackknife procedure on the GCL statistics. The manuscript is accompanied by a description of a custom-built Python package for calculating the GCL. These results provide practical guidelines for properly pre-processing and applying the GCL measure in transcriptional data.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9085802PMC
http://dx.doi.org/10.1038/s41598-022-11507-yDOI Listing

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