Starfysh integrates spatial transcriptomic and histologic data to reveal heterogeneous tumor–immune hubs

Author:

He Siyu,Jin YinuoORCID,Nazaret AchilleORCID,Shi Lingting,Chen XueerORCID,Rampersaud ShamORCID,Dhillon Bahawar S.ORCID,Valdez Izabella,Friend Lauren E.,Fan Joy Linyue,Park Cameron Y.,Mintz Rachel L.,Lao Yeh-HsingORCID,Carrera David,Fang Kaylee W.,Mehdi Kaleem,Rohde Madeline,McFaline-Figueroa José L.ORCID,Blei David,Leong Kam W.,Rudensky Alexander Y.ORCID,Plitas GeorgeORCID,Azizi ElhamORCID

Abstract

AbstractSpatially resolved gene expression profiling provides insight into tissue organization and cell–cell crosstalk; however, sequencing-based spatial transcriptomics (ST) lacks single-cell resolution. Current ST analysis methods require single-cell RNA sequencing data as a reference for rigorous interpretation of cell states, mostly do not use associated histology images and are not capable of inferring shared neighborhoods across multiple tissues. Here we present Starfysh, a computational toolbox using a deep generative model that incorporates archetypal analysis and any known cell type markers to characterize known or new tissue-specific cell states without a single-cell reference. Starfysh improves the characterization of spatial dynamics in complex tissues using histology images and enables the comparison of niches as spatial hubs across tissues. Integrative analysis of primary estrogen receptor (ER)-positive breast cancer, triple-negative breast cancer (TNBC) and metaplastic breast cancer (MBC) tissues led to the identification of spatial hubs with patient- and disease-specific cell type compositions and revealed metabolic reprogramming shaping immunosuppressive hubs in aggressive MBC.

Publisher

Springer Science and Business Media LLC

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