Robust mapping of spatiotemporal trajectories and cell–cell interactions in healthy and diseased tissues

Author:

Pham Duy,Tan Xiao,Balderson BradORCID,Xu JunORCID,Grice Laura F.ORCID,Yoon Sohye,Willis Emily F.,Tran Minh,Lam Pui YengORCID,Raghubar Arti,Kalita-de Croft PriyakshiORCID,Lakhani SunilORCID,Vukovic JanaORCID,Ruitenberg Marc J.ORCID,Nguyen Quan H.ORCID

Abstract

AbstractSpatial transcriptomics (ST) technologies generate multiple data types from biological samples, namely gene expression, physical distance between data points, and/or tissue morphology. Here we developed three computational-statistical algorithms that integrate all three data types to advance understanding of cellular processes. First, we present a spatial graph-based method, pseudo-time-space (PSTS), to model and uncover relationships between transcriptional states of cells across tissues undergoing dynamic change (e.g. neurodevelopment, brain injury and/or microglia activation, and cancer progression). We further developed a spatially-constrained two-level permutation (SCTP) test to study cell-cell interaction, finding highly interactive tissue regions across thousands of ligand-receptor pairs with markedly reduced false discovery rates. Finally, we present a spatial graph-based imputation method with neural network (stSME), to correct for technical noise/dropout and increase ST data coverage. Together, the algorithms that we developed, implemented in the comprehensive and fast stLearn software, allow for robust interrogation of biological processes within healthy and diseased tissues.

Funder

Department of Health | National Health and Medical Research Council

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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