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Molecular portraits of colorectal cancer morphological regions

Heterogeneity of colorectal carcinoma (CRC) represents a major hurdle towards personalized medicine. Efforts based on whole tumor profiling demonstrated that the CRC molecular subtypes were associated with specific tumor morphological patterns representing tumor subregions. We hypothesize that whole...

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Autores principales: Budinská, Eva, Hrivňáková, Martina, Ivkovic, Tina Catela, Madrzyk, Marie, Nenutil, Rudolf, Bencsiková, Beatrix, Al Tukmachi, Dagmar, Ručková, Michaela, Zdražilová Dubská, Lenka, Slabý, Ondřej, Feit, Josef, Dragomir, Mihnea-Paul, Borilova Linhartova, Petra, Tejpar, Sabine, Popovici, Vlad
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10642970/
https://www.ncbi.nlm.nih.gov/pubmed/37956043
http://dx.doi.org/10.7554/eLife.86655
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author Budinská, Eva
Hrivňáková, Martina
Ivkovic, Tina Catela
Madrzyk, Marie
Nenutil, Rudolf
Bencsiková, Beatrix
Al Tukmachi, Dagmar
Ručková, Michaela
Zdražilová Dubská, Lenka
Slabý, Ondřej
Feit, Josef
Dragomir, Mihnea-Paul
Borilova Linhartova, Petra
Tejpar, Sabine
Popovici, Vlad
author_facet Budinská, Eva
Hrivňáková, Martina
Ivkovic, Tina Catela
Madrzyk, Marie
Nenutil, Rudolf
Bencsiková, Beatrix
Al Tukmachi, Dagmar
Ručková, Michaela
Zdražilová Dubská, Lenka
Slabý, Ondřej
Feit, Josef
Dragomir, Mihnea-Paul
Borilova Linhartova, Petra
Tejpar, Sabine
Popovici, Vlad
author_sort Budinská, Eva
collection PubMed
description Heterogeneity of colorectal carcinoma (CRC) represents a major hurdle towards personalized medicine. Efforts based on whole tumor profiling demonstrated that the CRC molecular subtypes were associated with specific tumor morphological patterns representing tumor subregions. We hypothesize that whole-tumor molecular descriptors depend on the morphological heterogeneity with significant impact on current molecular predictors. We investigated intra-tumor heterogeneity by morphology-guided transcriptomics to better understand the links between gene expression and tumor morphology represented by six morphological patterns (morphotypes): complex tubular, desmoplastic, mucinous, papillary, serrated, and solid/trabecular. Whole-transcriptome profiling by microarrays of 202 tumor regions (morphotypes, tumor-adjacent normal tissue, supportive stroma, and matched whole tumors) from 111 stage II-IV CRCs identified morphotype-specific gene expression profiles and molecular programs and differences in their cellular buildup. The proportion of cell types (fibroblasts, epithelial and immune cells) and differentiation of epithelial cells were the main drivers of the observed disparities with activation of EMT and TNF-α signaling in contrast to MYC and E2F targets signaling, defining major gradients of changes at molecular level. Several gene expression-based (including single-cell) classifiers, prognostic and predictive signatures were examined to study their behavior across morphotypes. Most exhibited important morphotype-dependent variability within same tumor sections, with regional predictions often contradicting the whole-tumor classification. The results show that morphotype-based tumor sampling allows the detection of molecular features that would otherwise be distilled in whole tumor profile, while maintaining histopathology context for their interpretation. This represents a practical approach at improving the reproducibility of expression profiling and, by consequence, of gene-based classifiers.
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spelling pubmed-106429702023-11-14 Molecular portraits of colorectal cancer morphological regions Budinská, Eva Hrivňáková, Martina Ivkovic, Tina Catela Madrzyk, Marie Nenutil, Rudolf Bencsiková, Beatrix Al Tukmachi, Dagmar Ručková, Michaela Zdražilová Dubská, Lenka Slabý, Ondřej Feit, Josef Dragomir, Mihnea-Paul Borilova Linhartova, Petra Tejpar, Sabine Popovici, Vlad eLife Cancer Biology Heterogeneity of colorectal carcinoma (CRC) represents a major hurdle towards personalized medicine. Efforts based on whole tumor profiling demonstrated that the CRC molecular subtypes were associated with specific tumor morphological patterns representing tumor subregions. We hypothesize that whole-tumor molecular descriptors depend on the morphological heterogeneity with significant impact on current molecular predictors. We investigated intra-tumor heterogeneity by morphology-guided transcriptomics to better understand the links between gene expression and tumor morphology represented by six morphological patterns (morphotypes): complex tubular, desmoplastic, mucinous, papillary, serrated, and solid/trabecular. Whole-transcriptome profiling by microarrays of 202 tumor regions (morphotypes, tumor-adjacent normal tissue, supportive stroma, and matched whole tumors) from 111 stage II-IV CRCs identified morphotype-specific gene expression profiles and molecular programs and differences in their cellular buildup. The proportion of cell types (fibroblasts, epithelial and immune cells) and differentiation of epithelial cells were the main drivers of the observed disparities with activation of EMT and TNF-α signaling in contrast to MYC and E2F targets signaling, defining major gradients of changes at molecular level. Several gene expression-based (including single-cell) classifiers, prognostic and predictive signatures were examined to study their behavior across morphotypes. Most exhibited important morphotype-dependent variability within same tumor sections, with regional predictions often contradicting the whole-tumor classification. The results show that morphotype-based tumor sampling allows the detection of molecular features that would otherwise be distilled in whole tumor profile, while maintaining histopathology context for their interpretation. This represents a practical approach at improving the reproducibility of expression profiling and, by consequence, of gene-based classifiers. eLife Sciences Publications, Ltd 2023-11-13 /pmc/articles/PMC10642970/ /pubmed/37956043 http://dx.doi.org/10.7554/eLife.86655 Text en © 2023, Budinská et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Cancer Biology
Budinská, Eva
Hrivňáková, Martina
Ivkovic, Tina Catela
Madrzyk, Marie
Nenutil, Rudolf
Bencsiková, Beatrix
Al Tukmachi, Dagmar
Ručková, Michaela
Zdražilová Dubská, Lenka
Slabý, Ondřej
Feit, Josef
Dragomir, Mihnea-Paul
Borilova Linhartova, Petra
Tejpar, Sabine
Popovici, Vlad
Molecular portraits of colorectal cancer morphological regions
title Molecular portraits of colorectal cancer morphological regions
title_full Molecular portraits of colorectal cancer morphological regions
title_fullStr Molecular portraits of colorectal cancer morphological regions
title_full_unstemmed Molecular portraits of colorectal cancer morphological regions
title_short Molecular portraits of colorectal cancer morphological regions
title_sort molecular portraits of colorectal cancer morphological regions
topic Cancer Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10642970/
https://www.ncbi.nlm.nih.gov/pubmed/37956043
http://dx.doi.org/10.7554/eLife.86655
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