← Reviews
Open AccessVollständige AnalyseJun 16, 2026

Fungal β-1,3-glucans: cell wall constituents modulating innate gut immunity

This narrative review describes mechanisms by which fungal β-1,3-glucans interact with intestinal immune receptors but provides no clinical efficacy data in humans to support therapeutic recommendations.

The question (PICO)
PopulationHumans or animal models exposed to fungal β-1,3-glucans via dietary or supplemental routes
InterventionFungal β-1,3-glucans (from Saccharomyces cerevisiae, Lentinula edodes, Ganoderma lucidum, among others)
VergleichNot applicable — narrative review with no defined control group
EndpunktIntestinal immune modulation (Dectin-1/TLR activation, cytokine production), microbiota composition, gut barrier integrity, clinical outcomes in inflammatory diseases and cancer
DEvidenz
Studie
Übersichtsarbeit
Effekt
Unzureichend
Zusammenfassung der Ergebnisse nach Endpunkt
EndpunktGradRichtungEffektStudien
Dectin-1 activation and NF-κB signalingD Günstigdescritivo; sem tamanho de efeito quantificado
Gut microbiota modulation (Lactobacillus/Bifidobacterium)D Günstigdescritivo; dados preclinicos; sem IC 95%
Intestinal barrier integrityD Unzureichendsem dados quantitativos reportados
CR3/NK-mediated antitumor cytotoxicityD Günstigdescritivo; modelos in vitro e murinos; sem IC 95%
SCFA production via colonic fermentationD Unzureichenddescritivo; sem magnitude quantificada em humanos
Clinical outcomes in inflammatory bowel diseaseD Unzureichendnao avaliado com RCTs nesta revisao
Efficacy as adjuvant in cancer immunotherapyD Unzureichendcitados estudos clinicos selecionados sem pooling; sem IC 95%
Dectin-1 activation and NF-κB signalingD
Richtung Günstig
Effektdescritivo; sem tamanho de efeito quantificado
Studien
Gut microbiota modulation (Lactobacillus/Bifidobacterium)D
Richtung Günstig
Effektdescritivo; dados preclinicos; sem IC 95%
Studien
Intestinal barrier integrityD
Richtung Unzureichend
Effektsem dados quantitativos reportados
Studien
CR3/NK-mediated antitumor cytotoxicityD
Richtung Günstig
Effektdescritivo; modelos in vitro e murinos; sem IC 95%
Studien
SCFA production via colonic fermentationD
Richtung Unzureichend
Effektdescritivo; sem magnitude quantificada em humanos
Studien
Clinical outcomes in inflammatory bowel diseaseD
Richtung Unzureichend
Effektnao avaliado com RCTs nesta revisao
Studien
Efficacy as adjuvant in cancer immunotherapyD
Richtung Unzureichend
Effektcitados estudos clinicos selecionados sem pooling; sem IC 95%
Studien

Kontext

β-1,3-glucans constitute 30–80% of the fungal cell wall and are absent in mammals, making them immunologically distinct targets. They interact with Dectin-1, TLRs, CR3, and other pattern recognition receptors in gut-associated lymphoid tissue. Whether dietary intake of these molecules produces measurable clinical benefits remains unanswered by robust evidence.

Was die Studie zeigte

The review compiles mechanistic evidence that fungal β-1,3-glucans activate Dectin-1, TLR2/TLR4, CR3, and LacCer on macrophages, neutrophils, and dendritic cells, triggering NF-κB, CARD9-Bcl10-Malt1, and MAP kinase pathways. Preclinical data indicate promotion of Lactobacillus and Bifidobacterium and suppression of opportunistic pathogens. No randomized clinical trial data with validated primary endpoints are presented with absolute numbers or confidence intervals. The direction of immunological effects is considered favorable in the reviewed models, but clinical magnitude in humans is not quantified.

Wie es durchgeführt wurde

Narrative review published in Nutrients (2026); no registered protocol, no reported systematic search strategy, no explicit inclusion/exclusion criteria. Synthesizes mechanistic literature, in vitro studies, animal models, and selected clinical trials without meta-analysis. Aggregate sample size is not applicable.

Effektgröße

No consolidated effect size with 95% CI is reported. Individual effects cited are extracted from heterogeneous studies without statistical pooling.

Einschränkungen

Narrative review with no formal risk-of-bias assessment (AMSTAR-2, RoB 2, or ROBINS-I tools were not applied). Absence of systematic selection criteria introduces publication bias and confirmation bias. Most evidence is preclinical (in vitro or murine models), and direct extrapolation to humans is not justified by the presented data. Heterogeneity in fungal sources, doses, administration routes, and studied populations precludes unified clinical conclusions.

In der klinischen Praxis

Clinicians should not change practice based on this review alone. Fungal β-1,3-glucans have an acceptable safety profile as a food component, but clinical efficacy in specific conditions requires confirmation by RCTs with validated endpoints. Monitoring of immunocompromised patients is prudent given the potential for inflammatory modulation.

Was noch fehlt

RCTs in humans with clinical primary endpoints (infection recurrence, validated inflammatory markers, measurable intestinal permeability) and standardized doses of fungal β-1,3-glucans are needed. Shotgun-sequencing microbiota studies linked to immunological outcomes in specific populations (IBD, oncology, immunocompromised) are the next research priority.

Quelle: DOI 10.3390/nu18111794 · 2026

Microbiota Weekly

Die Mikrobiota-Evidenz der Woche, in Ihrer Sprache. Strukturierte Zusammenfassungen, rückverfolgbar zur Quelle.

Mit dem Abonnement stimmen Sie zu, E-Mails vom Microbiota.org-Institut zu erhalten. Jederzeit abbestellbar.