Spatial architecture of high-grade glioma reveals tumor heterogeneity within distinct domains

Author:

Moffet Joel J D12,Fatunla Oluwaseun E12,Freytag Lutz1,Kriel Jurgen12,Jones Jordan J3,Roberts-Thomson Samuel J4,Pavenko Anna5,Scoville David K5,Zhang Liang5,Liang Yan5,Morokoff Andrew P3,Whittle James R126,Freytag Saskia12,Best Sarah A12ORCID

Affiliation:

1. Personalised Oncology Division, The Walter and Eliza Hall Institute of Medical Research , Melbourne, Victoria , Australia

2. Department of Medical Biology, University of Melbourne , Melbourne, Victoria , Australia

3. Department of Surgery, Royal Melbourne Hospital , Melbourne, Victoria , Australia

4. Department of Anatomical Pathology, Royal Melbourne Hospital , Melbourne, Victoria , Australia

5. NanoString Technologies Inc. , Seattle, Washington , USA

6. Department of Medical Oncology, Peter MacCallum Cancer Centre , Melbourne, Victoria , Australia

Abstract

Abstract Background High-grade gliomas (HGGs) are aggressive primary brain cancers with poor response to standard regimens, driven by immense heterogeneity. In isocitrate dehydrogenase (IDH) wild-type HGG (glioblastoma, GBM), increased intratumoral heterogeneity is associated with more aggressive disease. Methods Spatial technologies can dissect complex heterogeneity within the tumor ecosystem by preserving cellular organization in situ. We employed GeoMx digital spatial profiling, CosMx spatial molecular imaging, Xenium in situ mapping and Visium spatial gene expression in experimental and validation patient cohorts to interrogate the transcriptional landscape in HGG. Results Here, we construct a high-resolution molecular map of heterogeneity in GBM and IDH-mutant patient samples to investigate the cellular communities that compose HGG. We uncovered striking diversity in the tumor landscape and degree of spatial heterogeneity within the cellular composition of the tumors. The immune distribution was diverse between samples, however, consistently correlated spatially with distinct tumor cell phenotypes, validated across tumor cohorts. Reconstructing the tumor architecture revealed two distinct niches, one composed of tumor cells that most closely resemble normal glial cells, associated with microglia, and the other niche populated by monocytes and mesenchymal tumor cells. Conclusions This primary study reveals high levels of intratumoral heterogeneity in HGGs, associated with a diverse immune landscape within spatially localized regions.

Funder

Cancer Australia

Victorian State Government Operational Infrastructure Support

Australian Government NHMRC Independent Research Institutes Infrastructure Support Scheme

the Victorian Cancer Agency Mid-Career Research Fellowship

WEHI Johnson PhD Scholarship

CSL Translational Data Science Scholarship and an Australian Government Research Training Program Scholarship

WEHI IPSI Scholarship

National Health and Medical Research Council

Publisher

Oxford University Press (OUP)

Subject

Surgery,Oncology,Neurology (clinical)

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