Spatial transcriptomics reveals discrete tumour microenvironments and autocrine loops within ovarian cancer subclones

Author:

Denisenko ElenaORCID,de Kock LeanneORCID,Tan Adeline,Beasley Aaron B.ORCID,Beilin Maria,Jones Matthew E.,Hou Rui,Muirí Dáithí Ó,Bilic Sanela,Mohan G. Raj K. A.,Salfinger Stuart,Fox SimonORCID,Hmon Khaing P. W.,Yeow YenORCID,Kim Youngmi,John Rhea,Gilderman Tami S.,Killingbeck EmilyORCID,Gray Elin S.ORCID,Cohen Paul A.ORCID,Yu Yu,Forrest Alistair R. R.ORCID

Abstract

AbstractHigh-grade serous ovarian carcinoma (HGSOC) is genetically unstable and characterised by the presence of subclones with distinct genotypes. Intratumoural heterogeneity is linked to recurrence, chemotherapy resistance, and poor prognosis. Here, we use spatial transcriptomics to identify HGSOC subclones and study their association with infiltrating cell populations. Visium spatial transcriptomics reveals multiple tumour subclones with different copy number alterations present within individual tumour sections. These subclones differentially express various ligands and receptors and are predicted to differentially associate with different stromal and immune cell populations. In one sample, CosMx single molecule imaging reveals subclones differentially associating with immune cell populations, fibroblasts, and endothelial cells. Cell-to-cell communication analysis identifies subclone-specific signalling to stromal and immune cells and multiple subclone-specific autocrine loops. Our study highlights the high degree of subclonal heterogeneity in HGSOC and suggests that subclone-specific ligand and receptor expression patterns likely modulate how HGSOC cells interact with their local microenvironment.

Funder

Department of Health | National Health and Medical Research Council

Cancer Council Western Australia

Cancer research trust

Publisher

Springer Science and Business Media LLC

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