Exploring the Unknown: How Can We Improve Single-cell RNAseq Cell Type Annotations in Non-model Organisms?

Integr Comp Biol

Department of Marine Biology and Ecology, Rosenstiel School of Marine, Atmospheric, and Earth Science, University of Miami, Miami, Florida, USA, 33149.

Published: November 2024

AI Article Synopsis

  • Single-cell RNA sequencing (scRNAseq) is crucial for identifying cell types in various multicellular organisms, but its standard methods are mainly tailored for model organisms like humans and mice, leading to difficulties with non-model species.
  • There are new strategies for annotating scRNAseq data in non-model organisms, including using evolutionary contexts and machine learning techniques that enable reference-free analyses.
  • Leveraging unannotated genes as potential cell markers can improve cell type identification in non-model organisms, fostering the discovery of novel cell types and deepening our understanding of cellular diversity.

Article Abstract

Single-cell RNA sequencing (scRNAseq) is a powerful tool to describe cell types in multicellular organisms across the animal kingdom. In standard scRNAseq analysis pipelines, clusters of cells with similar transcriptional signatures are given cell type labels based on marker genes that infer specialized known characteristics. Since these analyses are designed for model organisms, such as humans and mice, problems arise when attempting to label cell types of distantly related, non-model species that have unique or divergent cell types. Consequently, this leads to limited discovery of novel species-specific cell types and potential mis-annotation of cell types in non-model species while using scRNAseq. To address this problem, we discuss recently published approaches that help annotate scRNAseq clusters for any non-model organism. We first suggest that annotating with an evolutionary context of cell lineages will aid in the discovery of novel cell types and provide a marker-free approach to compare cell types across distantly related species. Secondly, machine learning has greatly improved bioinformatic analyses, so we highlight some open-source programs that use reference-free approaches to annotate cell clusters. Lastly, we propose the use of unannotated genes as potential cell markers for non-model organisms, as many do not have fully annotated genomes and these data are often disregarded. Improving single-cell annotations will aid the discovery of novel cell types and enhance our understanding of non-model organisms at a cellular level. By unifying approaches to annotate cell types in non-model organisms, we can increase the confidence of cell annotation label transfer and the flexibility to discover novel cell types.

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Source
http://dx.doi.org/10.1093/icb/icae112DOI Listing

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