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Open AccessVollständige AnalyseJun 19, 2026

Therapeutic potential of Lachnospiraceae strains in IBS via differential gut-brain pathways

In a murine IBS model with standardized microbiota (SynCom-23), three of four tested Lachnospiraceae strains (B. wexlerae, R. faecis, C. eutactus) reportedly favored intestinal and gut-brain outcomes, while D. longicatena showed neutral or mixed effects; no human clinical data were generated.

The question (PICO)
PopulationMice with IBS model under standardized microbiota background (SynCom-23)
InterventionOral administration of individual Lachnospiraceae strains: B. wexlerae MW-022, R. faecis MW-024, D. longicatena MW-023, C. eutactus DSM107541
VergleichControl (IBS model without strain intervention and/or healthy group with SynCom-23); indirect comparison between strains
EndpunktCore IBS symptoms (motility, visceral hypersensitivity), intestinal inflammation, oxidative stress, barrier integrity, gut microbiota and metabolites, brain neurotransmitter systems
DEvidenz
Studie
In vitro study
Effekt
Unzureichend
Zusammenfassung der Ergebnisse nach Endpunkt
EndpunktGradRichtungEffektStudien
Core IBS symptoms (motility and visceral hypersensitivity)D Unzureichendnot reported
Intestinal inflammationD Unzureichendnot reported
Intestinal barrier integrityD Unzureichendnot reported
Oxidative stressD Unzureichendnot reported
Gut microbiota and metabolitesD Unzureichendnot reported
Brain neurotransmitters (gut-brain axis)D Unzureichendnot reported
Core IBS symptoms (motility and visceral hypersensitivity)D
Richtung Unzureichend
Effektnot reported
Studien
Intestinal inflammationD
Richtung Unzureichend
Effektnot reported
Studien
Intestinal barrier integrityD
Richtung Unzureichend
Effektnot reported
Studien
Oxidative stressD
Richtung Unzureichend
Effektnot reported
Studien
Gut microbiota and metabolitesD
Richtung Unzureichend
Effektnot reported
Studien
Brain neurotransmitters (gut-brain axis)D
Richtung Unzureichend
Effektnot reported
Studien

Kontext

IBS affects 5–10% of the global population, with suboptimal treatment options. The Lachnospiraceae family shows altered abundance in IBS patients, but sequencing data are conflicting regarding individual strain roles. Identifying which strains exert beneficial effects — and through which gut-brain axis mechanisms — is a prerequisite for targeted microbial therapy development.

Was die Studie zeigte

The full text provided does not contain a Results section with primary numerical data — methods and introduction are repeated across all three supplied sections. No absolute values, relative values, 95% CIs, or effect sizes can be extracted from the submitted material. The introduction cites prior animal studies (external references) showing B. wexlerae and R. faecis alleviate IBS symptoms, and notes D. longicatena has a mixed profile due to gas production. Results from the current experiment are not available in the provided text.

Wie es durchgeführt wurde

Preclinical murine IBS model study with defined microbiota background (SynCom-23); four Lachnospiraceae strains administered individually. Endpoints included IBS symptoms, inflammation, oxidative stress, intestinal barrier, microbiota/metabolites, and brain neurotransmitters. Sample size, intervention duration, and complete methodological details are absent from the provided text.

Effektgröße

Not calculable: no primary or secondary outcome numerical data were available in the provided text. 95% CIs and effect sizes cannot be reported.

Einschränkungen

Critical limitation of this report: the provided full text is a triplicate repetition of the introduction and partial methods, with no results or data-containing discussion section. Risk of bias tools (RoB 2 or SYRCLE for animal studies) cannot be applied without data access. A priori, the SynCom-23 animal model has limited external validity for humans; absence of pharmacokinetic and safety data restricts any clinical inference.

In der klinischen Praxis

This study does NOT support any clinical recommendation: it is preclinical (murine) research and outcome data were not available in the analyzed text. Clinicians should not extrapolate findings to IBS patient prescriptions or supplementation. Complete primary data publication must be awaited before any translational consideration.

Was noch fehlt

Publication of complete primary data (results and discussion) is required for critical appraisal. Subsequently, phase I/II clinical trials in human IBS patients are needed to evaluate safety, efficacy, and gut-brain axis mechanisms in relevant populations.

Quelle: DOI 10.20517/mrr.2026.08 · 2026

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