# Evidence Summary

### Urolithin A Research Overview

1. Broad preclinical evidence across colorectal, pancreatic, prostate, breast, glioblastoma, liver, bladder, and lung cancer models
2. Repeated mechanistic findings around mitophagy, apoptosis, inflammatory signalling, tumour metabolism, and pathway suppression
3. In vivo tumour-growth and sensitisation signals in selected pancreatic, colorectal, and prostate models
4. Early human oncology interest, especially in prostate cancer and immune-related studies
5. No phase III oncology trials and no established cancer-treatment role at present

### Clinical Application Status

**Approved status:** Marketed as a supplement ingredient, not an approved cancer therapy.

**Clinical use:** Best positioned as an investigational adjunctive compound.

**Evidence strength:** Strong mechanistic and preclinical interest, with early human safety and emerging oncology-relevant clinical data.

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> Urolithin A has a credible preclinical oncology story. It appears to act across mitochondrial quality control, tumour signalling, immune function, and treatment-sensitisation pathways. That breadth makes it worth tracking. It does not yet make it a proven cancer treatment. The most honest position today is investigational adjunctive use, especially where immune function, mitophagy, or metabolic stress are part of the discussion.
> {% endstep %}
> {% endstepper %}

### Key Advantages

1. **Mitophagy relevance** — one of the clearest biological angles for Urolithin A is mitochondrial quality control
2. **Multi-pathway signalling effects** — recurrent findings involve PI3K/AKT/mTOR, Wnt/β-catenin, NF-κB, MAPK, and apoptosis pathways
3. **Direct supplementation bypasses microbiome variability** — oral Urolithin A avoids the problem of poor individual conversion from diet alone
4. **Early immune signal** — emerging work suggests relevance to NK cells, CD8-positive T-cell function, and checkpoint-combination research
5. **Good short-term human tolerability** — available human studies suggest favourable safety at commonly studied oral doses

### Key Considerations

1. **Human oncology data remains early** — most anticancer evidence is still cell and animal level
2. **Dose translation is unresolved** — laboratory concentrations cannot be mapped casually onto real-world oral dosing
3. **Combination questions remain open** — preclinical synergy signals are promising, but clinical interaction and timing data are still limited
4. **ER-positive context needs care** — selective estrogen receptor modulation signals make interpretation more cautious in hormone-sensitive disease
5. **Drug-handling uncertainty remains** — mechanistic interaction concerns exist, but formal oncology drug-interaction data is limited

### Bottom Line

Urolithin A is a serious investigational compound with meaningful oncology interest.

Its strongest case today rests on mechanistic credibility, mitophagy relevance, immune interest, and broad preclinical consistency.

Its main limit is still the same one that applies to many promising compounds in this library: human oncology proof remains early.

### In this section

* [Overview](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology.md)
* [Evidence Summary](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/evidence-summary.md)
* [Anticancer Mechanisms](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/anticancer-mechanisms.md)
* [Immune Effects](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/immune-effects.md)
* [Synergistic Combinations](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/synergistic-combinations.md)
* [Urolithin A Evidence by Cancer Type](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/urolithin-a-evidence-by-cancer-type.md)
* [Pharmacokinetics & Metabolism](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/pharmacokinetics-and-metabolism.md)
* [Safety & Interactions](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/safety-and-interactions.md)
* [Dosing & Timing](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/dosing-and-timing.md)
* [Sourcing Quality Urolithin A](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/sourcing-quality-urolithin-a.md)
* [Sensitisation to Conventional Therapies](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/sensitisation-to-conventional-therapies.md)
* [Antimicrobial, Antiviral & Terrain Support](/myhealingcommunity-docs/natural-medicines/urolithin-a-in-oncology/antimicrobial-antiviral-and-terrain-support.md)

### Key References

Urolithin A research overview and oncology applications\
<https://pmc.ncbi.nlm.nih.gov/articles/PMC12188533/>

Urolithin A in pancreatic cancer models and combination research\
<https://aacrjournals.org/mct/article/18/2/301/168585/Urolithin-A-a-Novel-Natural-Compound-to-Target>

Human safety, absorption, and plasma exposure of oral Urolithin A\
<https://pmc.ncbi.nlm.nih.gov/articles/PMC10460156/>

Immune relevance and early human NK-cell findings\
<https://www.frontiersin.org/journals/pharmacology/articles/10.3389/fphar.2024.1503317/full>

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This information is for education only. It is not medical advice, diagnosis, or treatment. Please speak with a qualified clinician before making changes to care, medication, or supplement use.
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© 2026 Abbey Mitchell. All rights reserved. Please share by URL rather than copying page text.
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