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Effect of the intratumoral microbiota on spatial and cellular heterogeneity in cancer

Authors :
Galeano Niño, Jorge Luis
Wu, Hanrui
LaCourse, Kaitlyn D.
Kempchinsky, Andrew G.
Baryiames, Alexander
Barber, Brittany
Futran, Neal
Houlton, Jeffrey
Sather, Cassie
Sicinska, Ewa
Taylor, Alison
Minot, Samuel S.
Johnston, Christopher D.
Bullman, Susan
Source :
Nature; November 2022, Vol. 611 Issue: 7937 p810-817, 8p
Publication Year :
2022

Abstract

The tumour-associated microbiota is an intrinsic component of the tumour microenvironment across human cancer types1,2. Intratumoral host–microbiota studies have so far largely relied on bulk tissue analysis1–3, which obscures the spatial distribution and localized effect of the microbiota within tumours. Here, by applying in situ spatial-profiling technologies4and single-cell RNA sequencing5to oral squamous cell carcinoma and colorectal cancer, we reveal spatial, cellular and molecular host–microbe interactions. We adapted 10x Visium spatial transcriptomics to determine the identity and in situ location of intratumoral microbial communities within patient tissues. Using GeoMx digital spatial profiling6, we show that bacterial communities populate microniches that are less vascularized, highly immuno‑suppressive and associated with malignant cells with lower levels of Ki-67 as compared to bacteria-negative tumour regions. We developed a single-cell RNA-sequencing method that we name INVADEseq (invasion–adhesion-directed expression sequencing) and, by applying this to patient tumours, identify cell-associated bacteria and the host cells with which they interact, as well as uncovering alterations in transcriptional pathways that are involved in inflammation, metastasis, cell dormancy and DNA repair. Through functional studies, we show that cancer cells that are infected with bacteria invade their surrounding environment as single cells and recruit myeloid cells to bacterial regions. Collectively, our data reveal that the distribution of the microbiota within a tumour is not random; instead, it is highly organized in microniches with immune and epithelial cell functions that promote cancer progression.

Details

Language :
English
ISSN :
00280836 and 14764687
Volume :
611
Issue :
7937
Database :
Supplemental Index
Journal :
Nature
Publication Type :
Periodical
Accession number :
ejs61164229
Full Text :
https://doi.org/10.1038/s41586-022-05435-0