Spatial transcriptomics at subspot resolution with BayesSpace

A tool for clustering analysis and resolution enhancement of spatial transcriptomics data
Spatial transcriptomics at subspot resolution with BayesSpace
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In recent years, there has been rapid development of spatial gene expression technology. The most mature of these are the closely related Spatial Transcriptomics and Visium platforms from 10x Genomics, which allow for gene expression profiling to be done with morphological context. Already, these spatial technologies have shown promise to generate novel biological insights in diverse areas such as cancer immunology and prefrontal cortex cytoarchitecture. However, the spatial technology is limited to resolution on the order of 10 cells per spot (the unit of observation for these data). In the meantime, development of analytical tools that effectively utilize the available spatial information and enhance the gene expression maps to higher resolution have lagged behind.

We developed BayesSpace to address these two primary challenges to clustering analysis of spatial expression data. BayesSpace models a low-dimensional representation of the gene expression using a multivariate t-distribution and then incorporates spatial context through the Potts model, which encourages neighboring spots to belong to the same cluster (Figure 1). This approach draws from well-established spatial statistics methods for image analysis. Effectively leveraging spatial information results in a massive improvement in clustering performance.

Potts model spatial prior
Figure 1. Potts model prior for Bayesian spatial modeling.

The principle of encouraging neighbors to belong to the same cluster can also be used to enhance the resolution of the spots to a “sub-spot” level. Here sub-spots are encouraged to belong to the same cluster. Sub-spot level expression cannot be directly observed, but can be estimated via MCMC by repeatedly nudging spot-level expression values. The details of this are available in the Methods of our paper. In practice, we find that enhanced resolution clustering can identify important biological structures that would otherwise be missed (Figure 2).

BayesSpace improves identification of biological features
Figure 2. At the subspot level, BayesSpace resolves finer stroma/tumor boundaries in an ovarian cancer sample and also identifies intra-tumoral regions with higher immune cell presence that are missed at the spot-level. Here, BayesSpace clusters are overlaid on the immunofluorescence image, which is used for validation. Three regions of interest from a tissue section are shown.

To make it easy for users to include BayesSpace in their analysis workflows, we designed BayesSpace to seamlessly integrate with existing analytical tools by using the SingleCellExperiment data structure. BayesSpace is available on Bioconductor.

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