Open AccessVollständige AnalyseJun 16, 2026

Microbial metabolomics and carcinogenesis: mechanistic pathways, clinical implications and methodological challenges

This narrative review maps associations between microbial metabolites and carcinogenesis but establishes no causality and provides no clinical intervention evidence.

The question (PICO)

PopulationBroad narrative review; no specific clinical population defined

InterventionMicrobial metabolomics as an analytical and mechanistic tool in carcinogenesis

EndpunktIdentification of mechanistic pathways and carcinogenesis biomarkers associated with microbial metabolites

DEvidenz

Studie

Übersichtsarbeit

Effekt

Unzureichend

Zusammenfassung der Ergebnisse nach Endpunkt

Endpunkt	Grad	Richtung	Effekt	Studien
Mechanistic pathways of carcinogenesis mediated by microbial metabolites	D	— Unzureichend	narrativo, sem quantificação	—
Conversion of primary to secondary bile acids by the bacterial bai operon	C	▲ Günstig	6 enzimas necessárias/suficientes; sem IC	1
Microbial carcinogenesis biomarkers (identification)	D	— Unzureichend	sem quantificação	—
Tumor microenvironment modulation by SCFAs	D	— Unzureichend	narrativo, sem quantificação	—
Applicability of LC-MS and NMR in oncological microbial metabolomics	D	— Unzureichend	descritivo, sem comparação quantitativa	—

Mechanistic pathways of carcinogenesis mediated by microbial metabolitesD

Richtung— Unzureichend

Effektnarrativo, sem quantificação

Studien—

Conversion of primary to secondary bile acids by the bacterial bai operonC

Richtung▲ Günstig

Effekt6 enzimas necessárias/suficientes; sem IC

Studien1

Microbial carcinogenesis biomarkers (identification)D

Richtung— Unzureichend

Effektsem quantificação

Studien—

Tumor microenvironment modulation by SCFAsD

Richtung— Unzureichend

Effektnarrativo, sem quantificação

Studien—

Applicability of LC-MS and NMR in oncological microbial metabolomicsD

Richtung— Unzureichend

Effektdescritivo, sem comparação quantitativa

Studien—

Kontext

Microbiome-derived metabolites (SCFAs, secondary bile acids, polyamines, amino acids) modulate inflammation, DNA integrity and the tumor microenvironment. These pathways are relevant to translational oncology. The absence of controlled clinical trials limits immediate clinical application.

Was die Studie zeigte

The review describes how microbial metabolites (e.g., secondary bile acids via the bai operon, SCFAs, polyamines) participate in carcinogenic pathways through inflammation, immune evasion and metabolic reprogramming. No effect sizes (RR, OR, SMD) or confidence intervals are reported, as no meta-analysis or primary quantitative analysis was performed. The key empirical contribution cited is the demonstration that six enzymes encoded in the bacterial bai operon are necessary and sufficient to convert primary to secondary bile acids, a capacity absent from the human genome.

Wie es durchgeführt wurde

Narrative review published in Frontiers in Cellular and Infection Microbiology (2026). No PROSPERO registration, systematic inclusion/exclusion criteria, or formal risk-of-bias assessment (AMSTAR-2 not applicable due to absence of quantitative synthesis). Covers analytical platforms (LC-MS, NMR) and mechanistic literature without defining a search time window or number of included studies.

Effektgröße

No effect size quantified. The study is descriptive; no 95% CI is reported for any outcome.

Einschränkungen

Narrative review without systematic methodology (no PRISMA; AMSTAR-2 not applicable): high risk of selection and confirmation bias. Does not distinguish causal evidence from association. Generalizes findings from preclinical models and small observational studies to the human context without quality weighting. Heterogeneity of populations, cancer types and analytical methodologies is not formally addressed.

In der klinischen Praxis

No change in clinical practice is supported by this study alone. Clinicians may use the text as a conceptual map of mechanistic pathways, not as a basis for prescription or screening. Microbial carcinogenesis biomarkers remain in a discovery phase, without prospective clinical validation.

Was noch fehlt

Prospective longitudinal studies and RCTs testing interventions targeting the microbial metabolome in primary oncological outcomes are needed. Standardization of analytical platforms (LC-MS vs NMR) and cohorts is a prerequisite for replicability.

Quelle: DOI 10.3389/fcimb.2026.1787954 · 2026

Microbial metabolomics and carcinogenesis: mechanistic pathways, clinical implications and methodological challenges

Kontext

Was die Studie zeigte

Wie es durchgeführt wurde

Effektgröße

Einschränkungen

In der klinischen Praxis

Was noch fehlt

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