According to the driver–passenger model for colorectal cancer (CRC), the tumor-associated microbiota is a dynamic ecosystem of bacterial species where bacteria with carcinogenic features linked to CRC initiation are defined as “drivers”, while opportunistic bacteria colonizing more advanced tumor stages are known as “passengers”. We reasoned that also gut microbiota-associated metabolites may be differentially enriched according to tumor stage, and be potential determinants of CRC development. Thus, we characterized the mucosa- and lumen-associated microbiota (MAM and LAM, respectively) and mucosa-associated metabolites in low- vs. high-grade dysplastic colon polyps from 78 patients. We show that MAM, obtained with a new biopsy-preserving approach, and LAM differ in composition and α/β-diversity. By stratifying patients for polyp histology, we found that bacteria proposed as passengers by previous studies colonized high-grade dysplastic adenomas, whereas driver taxa were enriched in low-grade polyps. Furthermore, we report altered “mucosa-associated metabolite” levels in low- vs. high-grade groups. Integrated microbiota-metabolome analysis suggests the involvement of the gut microbiota in the production and consumption of these metabolites. Altogether, our findings support the involvement of bacterial species and associated metabolites in CRC mucosal homeostasis in a tumor-stage-specific manner. These distinct signatures may be used to distinguish low-grade from high-grade dysplastic polyps.

Distinct Signatures of Tumor-Associated Microbiota and Metabolome in Low-Grade vs. High-Grade Dysplastic Colon Polyps: Inference of Their Role in Tumor Initiation and Progression / Clavenna, Michela Giulia; La Vecchia, Marta; Sculco, Marika; Joseph, Soni; Barberis, Elettra; Amede, Elia; Mellai, Marta; Brossa, Silvia; Borgonovi, Giulia; Occhipinti, Pietro; Boldorini, Renzo; Robotti, Elisa; Azzimonti, Barbara; Bona, Elisa; Pasolli, Edoardo; Ferrante, Daniela; Manfredi, Marcello; Aspesi, Anna; Dianzani, Irma. - In: CANCERS. - ISSN 2072-6694. - 15:12(2023), p. 3065. [10.3390/cancers15123065]

Distinct Signatures of Tumor-Associated Microbiota and Metabolome in Low-Grade vs. High-Grade Dysplastic Colon Polyps: Inference of Their Role in Tumor Initiation and Progression

Pasolli, Edoardo;
2023

Abstract

According to the driver–passenger model for colorectal cancer (CRC), the tumor-associated microbiota is a dynamic ecosystem of bacterial species where bacteria with carcinogenic features linked to CRC initiation are defined as “drivers”, while opportunistic bacteria colonizing more advanced tumor stages are known as “passengers”. We reasoned that also gut microbiota-associated metabolites may be differentially enriched according to tumor stage, and be potential determinants of CRC development. Thus, we characterized the mucosa- and lumen-associated microbiota (MAM and LAM, respectively) and mucosa-associated metabolites in low- vs. high-grade dysplastic colon polyps from 78 patients. We show that MAM, obtained with a new biopsy-preserving approach, and LAM differ in composition and α/β-diversity. By stratifying patients for polyp histology, we found that bacteria proposed as passengers by previous studies colonized high-grade dysplastic adenomas, whereas driver taxa were enriched in low-grade polyps. Furthermore, we report altered “mucosa-associated metabolite” levels in low- vs. high-grade groups. Integrated microbiota-metabolome analysis suggests the involvement of the gut microbiota in the production and consumption of these metabolites. Altogether, our findings support the involvement of bacterial species and associated metabolites in CRC mucosal homeostasis in a tumor-stage-specific manner. These distinct signatures may be used to distinguish low-grade from high-grade dysplastic polyps.
2023
Distinct Signatures of Tumor-Associated Microbiota and Metabolome in Low-Grade vs. High-Grade Dysplastic Colon Polyps: Inference of Their Role in Tumor Initiation and Progression / Clavenna, Michela Giulia; La Vecchia, Marta; Sculco, Marika; Joseph, Soni; Barberis, Elettra; Amede, Elia; Mellai, Marta; Brossa, Silvia; Borgonovi, Giulia; Occhipinti, Pietro; Boldorini, Renzo; Robotti, Elisa; Azzimonti, Barbara; Bona, Elisa; Pasolli, Edoardo; Ferrante, Daniela; Manfredi, Marcello; Aspesi, Anna; Dianzani, Irma. - In: CANCERS. - ISSN 2072-6694. - 15:12(2023), p. 3065. [10.3390/cancers15123065]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11588/925563
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