Abstract Summary Recent years have seen the release of several toolsets that reveal cell-cell interactions from single-cell data. However, all existing approaches leverage mean celltype gene expression values, and do not preserve the single-cell fidelity of the original data. Here, we present NICHES ( N iche I nteractions and C ommunication H eterogeneity in E xtracellular S ignaling), a tool to explore extracellular signaling at the truly single-cell level. NICHES allows embedding of ligand-receptor signal proxies to visualize heterogeneous signaling archetypes within cell clusters, between cell clusters, and across experimental conditions. When applied to spatial transcriptomic data, NICHES can be used to reflect local cellular microenvironment. NICHES can operate with any list of ligand-receptor signaling mechanisms and is compatible with existing single-cell packages and pseudotime techniques. NICHES is also a user friendly and extensible program, allowing rapid analysis of cell-cell signaling at single-cell resolution. Availability and implementation NICHES is an open-source software implemented in R under academic free license v3.0 and it is available at github.com/msraredon/NICHES. Use-case vignettes are available at https://msraredon.github.io/NICHES/ . Contact michasam.raredon@yale.edu ; yuval.kluger@yale.edu
This paper's license is marked as closed access or non-commercial and cannot be viewed on ResearchHub. Visit the paper's external site.