Multi-omics machine learning to study host-microbiome interactions in early-onset colorectal cancer-Reference-Cited by-同舟云学术

Multi-omics machine learning to study host-microbiome interactions in early-onset colorectal cancer

Published:2024-07-17 Issue:1 Volume:8 Page:
ISSN:2397-768X
Container-title:npj Precision Oncology
language:en
Short-container-title:npj Precis. Onc.

Author:

Jayakrishnan Thejus T.^ORCID,Sangwan Naseer,Barot Shimoli V.^ORCID,Farha Nicole,Mariam Arshiya,Xiang Shao,Aucejo Federico,Conces Madison,Nair Kanika G.,Krishnamurthi Smitha S.,Schmit Stephanie L.,Liska David,Rotroff Daniel M.,Khorana Alok A.,Kamath Suneel D.^ORCID

Abstract

AbstractThe incidence of early-onset colorectal cancer (eoCRC) is rising, and its pathogenesis is not completely understood. We hypothesized that machine learning utilizing paired tissue microbiome and plasma metabolome features could uncover distinct host-microbiome associations between eoCRC and average-onset CRC (aoCRC). Individuals with stages I–IV CRC (n = 64) were categorized as eoCRC (age ≤ 50, n = 20) or aoCRC (age ≥ 60, n = 44). Untargeted plasma metabolomics and 16S rRNA amplicon sequencing (microbiome analysis) of tumor tissue were performed. We fit DIABLO (Data Integration Analysis for Biomarker Discovery using Latent variable approaches for Omics studies) to construct a supervised machine-learning classifier using paired multi-omics (microbiome and metabolomics) data and identify associations unique to eoCRC. A differential association network analysis was also performed. Distinct clustering patterns emerged in multi-omic dimension reduction analysis. The metabolomics classifier achieved an AUC of 0.98, compared to AUC 0.61 for microbiome-based classifier. Circular correlation technique highlighted several key associations. Metabolites glycerol and pseudouridine (higher abundance in individuals with aoCRC) had negative correlations with Parasutterella, and Ruminococcaceae (higher abundance in individuals with eoCRC). Cholesterol and xylitol correlated negatively with Erysipelatoclostridium and Eubacterium, and showed a positive correlation with Acidovorax with higher abundance in individuals with eoCRC. Network analysis revealed different clustering patterns and associations for several metabolites e.g.: urea cycle metabolites and microbes such as Akkermansia. We show that multi-omics analysis can be utilized to study host-microbiome correlations in eoCRC and demonstrates promising biomarker potential of a metabolomics classifier. The distinct host-microbiome correlations for urea cycle in eoCRC may offer opportunities for therapeutic interventions.

Funder

The Sondra and Stephen Hardis Chair in Oncology Research

Publisher

Springer Science and Business Media LLC

Link

https://www.nature.com/articles/s41698-024-00647-1.pdf

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