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  3. Profiling the heterogeneity of colorectal cancer consensus molecular subtypes using spatial transcriptomics.
 

Profiling the heterogeneity of colorectal cancer consensus molecular subtypes using spatial transcriptomics.

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BORIS DOI
10.48350/191475
Date of Publication
January 10, 2024
Publication Type
Article
Division/Institute

Institut für Tierpath...

Institut für Tierpath...

Contributor
Valdeolivas, Alberto
Amberg, Bettina Katharinaorcid-logo
Institut für Tierpathologie (ITPA)
Giroud, Nicolas
Richardson, Marion
Gálvez, Eric J C
Badillo, Solveig
Julien-Laferrière, Alice
Túrós, Péter Demeter
Institut für Tierpathologie (ITPA) - Labortierpathologie
Institut für Tierpathologie (ITPA)
Voith von Voithenberg, Lena
Wells, Isabelle
Pesti, Benedek
Lo, Amy A
Yángüez, Emilio
Das Thakur, Meghna
Bscheider, Michael
Sultan, Marc
Kumpesa, Nadine
Jacobsen, Björn
Bergauer, Tobias
Saez-Rodriguez, Julio
Rottenberg, Svenorcid-logo
Institut für Tierpathologie (ITPA)
Schwalie, Petra C
Hahn, Kerstin
Subject(s)

600 - Technology::630...

Series
NPJ precision oncology
ISSN or ISBN (if monograph)
2397-768X
Publisher
Springer Nature
Language
English
Publisher DOI
10.1038/s41698-023-00488-4
PubMed ID
38200223
Description
The consensus molecular subtypes (CMS) of colorectal cancer (CRC) is the most widely-used gene expression-based classification and has contributed to a better understanding of disease heterogeneity and prognosis. Nevertheless, CMS intratumoral heterogeneity restricts its clinical application, stressing the necessity of further characterizing the composition and architecture of CRC. Here, we used Spatial Transcriptomics (ST) in combination with single-cell RNA sequencing (scRNA-seq) to decipher the spatially resolved cellular and molecular composition of CRC. In addition to mapping the intratumoral heterogeneity of CMS and their microenvironment, we identified cell communication events in the tumor-stroma interface of CMS2 carcinomas. This includes tumor growth-inhibiting as well as -activating signals, such as the potential regulation of the ETV4 transcriptional activity by DCN or the PLAU-PLAUR ligand-receptor interaction. Our study illustrates the potential of ST to resolve CRC molecular heterogeneity and thereby help advance personalized therapy.
Handle
https://boris-portal.unibe.ch/handle/20.500.12422/173273
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FileFile TypeFormatSizeLicensePublisher/Copright statementContent
s41698-023-00488-4.pdftextAdobe PDF7.6 MBpublishedOpen
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