Systematic review links gut microbial metabolites to colitis-associated colorectal cancer risk

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Frontiers in Medicine Published May 4, 2026 Medically reviewed May 4, 2026 DOI ↗ By Dr. Amelia Tan, PhD · Internal Medicine & Chronic Disease

Key Takeaway

Consider that elevated TMAO levels are associated with worse outcomes in colitis-associated colorectal cancer, but causality is unproven.

This systematic review examines the role of gut microbial metabolites in colitis-associated colorectal cancer (CAC) and inflammatory bowel disease. The review covers metabolites including short-chain fatty acids, succinate, secondary bile acids, TMAO, tryptophan metabolites, polyamines, hydrogen sulfide, and vitamin B2. The authors synthesize evidence from multiple studies, primarily focusing on associations between these metabolites and disease outcomes.

Key findings indicate that elevated plasma TMAO levels are closely associated with poor survival outcomes, including increased risks of all-cause mortality and recurrence. However, the review does not provide pooled effect sizes or quantitative analyses, as it is a narrative synthesis. The evidence is based on associations, and causal relationships between metabolites and disease are not established.

The authors acknowledge several limitations, including interindividual microbial heterogeneity, the challenge of establishing causal links, and the need for optimization of clinical intervention pathways. The review highlights that gut microbial metabolites offer new paradigms for early diagnostic biomarkers and targeted therapies, but these remain exploratory.

For clinicians, this review underscores the potential of microbial metabolites as biomarkers in CAC but emphasizes that the evidence is preliminary. No specific clinical recommendations can be made at this time. Further research is needed to validate these associations and translate them into clinical practice.

Study Details

Study typeSystematic review

EvidenceLevel 1

PublishedMay 2026

View Original Abstract ↓

Colitis-associated colorectal cancer (CAC) represents the most severe malignant complication of inflammatory bowel disease (IBD), characterized by high invasiveness, frequent recurrence, and poor prognosis. Recent studies have revealed that gut microbial metabolites are involved in the initiation and progression of CAC through a “metabolite-signaling pathway-epigenetics” regulatory network, demonstrating a remarkable dual modulatory role. Protective metabolites, such as short-chain fatty acids (SCFAs), tryptophan derivatives (e.g., indole compounds), and vitamin B2, exert anti-inflammatory, antioxidant, intestinal barrier-enhancing, and oncogenic pathway-suppressing effects. In contrast, pathogenic metabolites promote carcinogenesis. Prominent among such metabolites are secondary bile acids [e.g., deoxycholic acid (DCA)], trimethylamine N-oxide (TMAO), and high concentrations of hydrogen sulfide (H2S). These metabolites activate nuclear factor κB (NF-κB), stimulate the release of pro-inflammatory cytokines, induce DNA damage, and disrupt immune homeostasis. Conversely, elevated plasma TMAO levels are closely associated with poor survival outcomes, with high-risk individuals showing significantly increased risks of all-cause mortality and recurrence. This review systematically summarizes the microbial origins, dual mechanisms in CAC, and potential therapeutic value of several key gut microbiota-derived metabolites, including SCFAs, succinate, secondary bile acids, TMAO, tryptophan metabolites, polyamines, H2S, and vitamin B2. Based on current evidence, intervention strategies are primarily focused on regulating microbial metabolic balance via probiotics/prebiotics, increasing precursor supply of beneficial metabolites through dietary fiber supplementation, reconstructing gut homeostasis via microbiota transplantation, and developing metabolite analogs or chelators for targeted intervention. Although gut microbial metabolites offer new paradigms for early diagnostic biomarkers and targeted therapies in CAC, clinical translation still faces several challenges, including interindividual microbial heterogeneity, establishment of causal relationships between metabolites and disease, and optimization of clinical intervention pathways, which require further research breakthroughs.