What is the Joe Tippens Protocol?

The Joe Tippens Protocol is an alternative cancer protocol that gained viral attention in 2019 after Joe Tippens claimed fenbendazole (a veterinary antiparasitic) helped cure his Stage 4 small cell lung cancer. The expanded protocol includes up to 8 compounds: fenbendazole, mebendazole, ivermectin, vitamin B17, FECO, methylene blue, TUDCA, and activated charcoal. It is not clinically validated and has zero completed human clinical trials.

Is there scientific evidence for the Joe Tippens Protocol?

The protocol is based on one viral anecdote plus preclinical (cell culture and animal) data. The key study is Dogra et al. 2018 in Scientific Reports, which showed fenbendazole anticancer mechanisms in NSCLC cells. There are no completed human clinical trials for fenbendazole as a cancer treatment, and no studies have evaluated the full protocol combination in humans.

Is fenbendazole FDA-approved for cancer?

No. Fenbendazole is not FDA-approved for any human use. It is approved only as a veterinary antiparasitic (brand names Panacur, Safe-Guard). No regulatory agency worldwide has approved fenbendazole for cancer treatment. All human use is off-label and experimental.

What are the risks of the Joe Tippens Protocol?

Risks include hepatotoxicity (liver damage), drug interactions via CYP450 enzymes, no established human safety data for the compound combination, potential interference with conventional cancer treatments, and risks specific to individual compounds like amygdalin (vitamin B17) which can release cyanide. There is no human safety data for this specific combination of compounds.

What is the original Joe Tippens dosing protocol?

The original community protocol involves fenbendazole 222mg daily (from 1g of Panacur paste) on a 3-days-on, 4-days-off cycle, combined with Vitamin E succinate 800 IU, curcumin 600mg, and CBD oil 25mg daily. This is a community-shared protocol, NOT medical advice, and has not been validated in clinical trials.

Joe Tippens Protocol: Complete Overview of the Alternative Cancer Research Stack

Origin Story

How It Started

One anecdote. Zero clinical trials. A viral movement.

Joe Tippens — The Viral Anecdote

In 2016, Joe Tippens was diagnosed with Stage 4 small cell lung cancer (SCLC) that had metastasized throughout his body. After a veterinarian friend suggested he try fenbendazole — an animal dewormer — Tippens began taking it alongside conventional treatment.

Tippens later reported complete remission and began sharing his story through a blog (MyCANCERstory.rocks) in 2019. The story went viral, particularly in South Korea where fenbendazole sales surged dramatically.

Critical context: Tippens was also receiving conventional cancer treatment (immunotherapy) during this period. His case is a single anecdote — not clinical evidence. Oncologists have noted that spontaneous remissions, while rare, do occur, and attributing his outcome solely to fenbendazole is scientifically unsupported.

The community protocol has since expanded well beyond Tippens' original regimen, with additional compounds added by various practitioners and patient communities. The “expanded stack” described on this page reflects the broader community protocol — not Tippens’ original combination.

The Stack

8 Compounds in the Protocol

Community-reported compounds and dosing. These are NOT medical recommendations. Doses shown reflect community protocols, not clinical guidelines.

💊

Fenbendazole

Primary • Benzimidazole

Veterinary antiparasitic (Panacur/Safe-Guard). The core compound of the original protocol. Targets microtubules, glucose uptake, and p53 pathways in preclinical studies.

Community dose: 222mg/day (from 1g Panacur paste), 3 days on / 4 days off

⚠️ NOT FDA-approved for human use

🔬

Mebendazole

Alternative • Benzimidazole

Human-approved antiparasitic (Vermox). Same drug class as fenbendazole. Some community members substitute it due to existing human safety data for antiparasitic use.

Community dose: 100–200mg/day, cycling varies

⚠️ FDA-approved for parasites only, NOT cancer

🧬

Ivermectin

Adjunct • Avermectin

Antiparasitic with preclinical anticancer signals. Some expanded protocols include it for potential synergy with benzimidazoles.

Community dose: 0.2–0.4mg/kg, intermittent dosing

⚠️ FDA-approved for parasites only, NOT cancer

⚗️

Vitamin B17 / Amygdalin

Controversial • Cyanogenic Glycoside

Derived from apricot kernels. Extremely controversial — can release cyanide during metabolism. The FDA has banned its sale as a cancer treatment. Multiple poisoning deaths reported.

Community dose: Varies widely — NO established safe dose

🚫 FDA BANNED as cancer treatment. Cyanide toxicity risk.

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FECO (Full Extract Cannabis Oil)

Adjunct • Cannabinoid

High-THC cannabis extract (also called RSO/Rick Simpson Oil). Preclinical data on cannabinoid-induced apoptosis. Legal status varies by jurisdiction.

Community dose: Gradual titration up to 1g/day

⚠️ NOT FDA-approved. Schedule I federal status (US)

🔵

Methylene Blue

Adjunct • Phenothiazine

Synthetic dye with mitochondrial effects. FDA-approved for methemoglobinemia only. Preclinical data suggests mitochondrial targeting in cancer cells.

Community dose: 0.5–1mg/kg, pharmaceutical grade

⚠️ FDA-approved for methemoglobinemia only

🛡️

TUDCA

Support • Bile Acid

Tauroursodeoxycholic acid — a liver-protective bile acid. Included as hepatoprotective support given that multiple protocol compounds carry hepatotoxicity risk.

Community dose: 250–500mg/day

⚠️ Sold as supplement. Not FDA-evaluated for this use.

⬛

Activated Charcoal

Support • Binder/Detox

Used as a binder to adsorb toxins and metabolites. Taken away from other compounds to avoid absorbing them. Common in detox protocols.

Community dose: 500–1000mg, 2 hours from other compounds

⚠️ OTC supplement. Can bind medications — timing critical.

Mechanisms

How Key Compounds Work (Preclinical Data)

All mechanisms shown are from cell culture and animal studies. None are confirmed in human cancer patients.

Fenbendazole — Triple Mechanism (Dogra 2018)

🔧 Microtubule disruption — Binds β-tubulin, destabilizes cytoskeleton, arrests mitosis
🚫 Glucose uptake inhibition — Downregulates GLUT4 transporters, starves cancer cells of glucose
🔬 p53 reactivation — Stabilizes wild-type p53 tumor suppressor protein, promotes apoptosis
🧪 Proteasome interference — May affect protein degradation pathways in cancer cells

Mebendazole — Shared Benzimidazole Pathways

🔧 Tubulin binding — Same drug class as fenbendazole, similar microtubule disruption
📉 Angiogenesis inhibition — May reduce new blood vessel formation to tumors (preclinical)
⚡ Hedgehog pathway — Preclinical data suggests inhibition of Hedgehog signaling in some cancers
🧬 Bcl-2 modulation — May shift pro/anti-apoptotic protein balance toward cell death

Ivermectin — Preclinical Anticancer Signals

🎯 WNT/TCF pathway — May inhibit WNT signaling involved in cancer cell proliferation
⚡ Mitochondrial dysfunction — Can induce oxidative stress selectively in cancer cells (in vitro)
🔄 Autophagy modulation — May alter cellular recycling pathways leading to cell death
🛑 MDR1 inhibition — Preclinical evidence of overcoming drug resistance mechanisms

Methylene Blue — Mitochondrial Targeting

⚡ Electron carrier — Alters mitochondrial electron transport chain dynamics
🔬 ROS generation — May increase reactive oxygen species selectively in cancer cells
🧬 Autophagy induction — Preclinical data on triggering autophagic cell death pathways
🎯 Photodynamic potential — Acts as photosensitizer under specific light wavelengths

Evidence Quality

Research Evidence by Compound

Honest assessment of where the science stands. Preclinical ≠ clinical. Animal data ≠ human proof.

Fenbendazole Preclinical: Strong

In vitro & animal modelsClinical: None

Mebendazole Preclinical: Strong

In vitro, animal, + limited case reportsClinical: Very Early

Ivermectin Preclinical: Moderate

In vitro studies, limited animal dataClinical: Minimal

Vitamin B17 / Amygdalin Preclinical: Weak

Outdated studies, safety concerns dominateClinical: Negative (toxic)

FECO / Cannabis Oil Preclinical: Moderate

Cannabinoid receptor studies, some animal dataClinical: Very Limited

Methylene Blue Preclinical: Emerging

In vitro mitochondrial studiesClinical: None for cancer

TUDCA As hepatoprotectant: Moderate

Well-studied for liver protectionClinical: For liver, not cancer

Activated Charcoal As binder: Established

Established adsorbent / poison control useClinical: For binding, not cancer

Safety

Safety & Risk Assessment

There is NO human safety data for this combination of compounds. Each carries individual risks that may compound when stacked.

⚠️ Hepatotoxicity (Liver Damage) HIGH RISK

Fenbendazole, mebendazole, and methylene blue all carry hepatotoxicity risk. Stacking multiple hepatotoxic compounds significantly increases liver damage potential. Regular LFT (liver function tests) strongly recommended.

⚠️ Drug Interactions (CYP450) HIGH RISK

Multiple compounds metabolized via CYP enzymes. Cannabis oil inhibits CYP3A4/CYP2C9. This can alter blood levels of fenbendazole, mebendazole, ivermectin, and any concurrent medications unpredictably.

🚫 Cyanide Toxicity (Vitamin B17) CRITICAL RISK

Amygdalin/B17 releases hydrogen cyanide during metabolism. Multiple deaths and poisonings documented. The FDA has banned its sale as a cancer treatment. This is the highest-risk compound in the stack.

⚠️ Serotonin Syndrome Risk MODERATE RISK

Methylene blue is an MAO inhibitor. Combined with SSRIs, SNRIs, or other serotonergic drugs, it can trigger life-threatening serotonin syndrome. Contraindicated with many common antidepressants.

⚠️ Medication Binding (Activated Charcoal) MODERATE RISK

Activated charcoal binds indiscriminately — including medications and other protocol compounds. Must be taken 2+ hours away from all other substances. Can reduce effectiveness of concurrent cancer treatments.

⚠️ Interference with Conventional Treatment HIGH RISK

Using unproven compounds instead of — or alongside — conventional cancer treatment can reduce treatment efficacy, cause dangerous interactions, or lead to treatment delays. Always involve your oncologist.

Variants

Community Protocol Variants

How different community versions of the protocol compare. None are clinically validated.

Component	Original Tippens	Expanded Stack	Mebendazole Sub
Fenbendazole	222mg, 3 on/4 off	222mg, 3 on/4 off	—
Mebendazole	—	Optional add	100–200mg daily
Curcumin	600mg daily	600mg daily	600mg daily
CBD Oil	25mg daily	Replaced by FECO	25mg daily
Vitamin E (succinate)	800 IU daily	800 IU daily	800 IU daily
Ivermectin	—	0.2–0.4mg/kg, intermittent	Optional
Vitamin B17	—	Varies (controversial)	—
FECO	—	Titrated to 1g/day	—
Methylene Blue	—	0.5–1mg/kg	—
TUDCA	—	250–500mg daily	250–500mg daily
Activated Charcoal	—	500–1000mg (timed)	Optional

Citations

Key Study References

Primary research papers for each compound. Links go to PubMed/Nature for verification.

1

Dogra N, Kumar A, Mukhopadhyay T. Fenbendazole acts as a moderate microtubule destabilizing agent and causes cancer cell death by modulating multiple cellular pathways. Sci Rep. 2018;8:11926. doi:10.1038/s41598-018-30158-6

2

Son DS, Lee ES, Bhatt DK. Anti-cancer effects of fenbendazole on 5-fluorouracil-resistant colorectal cancer cells. Korean J Parasitol. 2022;60(5):377-387. PMC9437363

3

Bai RY, Staedtke V, Aprhys CM, Gallia GL, Riggins GJ. Antiparasitic mebendazole shows survival benefit in 2 preclinical models of glioblastoma multiforme. Neuro Oncol. 2011;13(9):974-982. PMID: 21764822

4

Pantziarka P, Bouche G, Meheus L, et al. Repurposing drugs in oncology (ReDO) — mebendazole as an anti-cancer agent. Ecancermedicalscience. 2014;8:443. PMID: 25075217

5

Juarez M, Schcolnik-Cabrera A, Duenas-Gonzalez A. The multitargeted drug ivermectin: from an antiparasitic agent to a repositioned cancer drug. Am J Cancer Res. 2018;8(2):317-331. PMID: 29516532

6

Velasco G, Sanchez C, Guzman M. Anticancer mechanisms of cannabinoids. Curr Oncol. 2016;23(Suppl 2):S23-S32. PMID: 27022311

7

Milankovic V, et al. Repositioning of Dog Dewormer: Fenbendazole Fever. Curr Issues Mol Biol. 2022;44(10):4977-4998. doi:10.3390/cimb44100338

8

Moertel CG, et al. A clinical trial of amygdalin (Laetrile) in the treatment of human cancer. N Engl J Med. 1982;306(4):201-206. PMID: 7033783 — Found no benefit + cyanide toxicity.

Summary

Key Takeaways

An honest look at what the evidence supports and what remains unknown.

✅ What We Know

✅ Fenbendazole shows multi-pathway anticancer activity in cell culture and animal models (Dogra 2018)
✅ Benzimidazoles (fenbendazole, mebendazole) disrupt microtubules similarly to some chemotherapy drugs
✅ Mebendazole has existing human safety data for antiparasitic use and limited case reports in cancer
✅ TUDCA has established hepatoprotective properties supported by clinical evidence
✅ Individual compounds have published preclinical anticancer data of varying quality
✅ Joe Tippens did achieve remission (though he was on concurrent immunotherapy)

⚠️ What We Don’t Know

⚠️ Whether any of these compounds work against cancer in humans at achievable doses
⚠️ Safety of combining 8 compounds with overlapping metabolic pathways
⚠️ Optimal dosing, cycling, or duration for any anticancer application
⚠️ How these compounds interact with standard cancer treatments (chemo, immunotherapy, radiation)
⚠️ Whether Tippens' remission was due to fenbendazole, immunotherapy, or spontaneous remission
⚠️ Long-term effects of benzimidazole use at these doses in humans
⚠️ Whether preclinical cancer cell kill translates to tumor reduction in living humans

Products

Related Products

Commonly used supplies. Links go to Amazon search results. Inclusion does not constitute endorsement or medical recommendation.

💉

Bacteriostatic Water

View on Amazon

🗑️

Sharps Container

View on Amazon

🛡️

TUDCA Supplement

View on Amazon

⬛

Activated Charcoal

View on Amazon

🟡

Curcumin Supplement

View on Amazon

Related Guides

Deep-Dive Into Each Compound

Detailed research guides for individual compounds in the protocol.

⚠️ Important Disclaimer

This page is for educational and informational purposes only. It does not constitute medical advice, diagnosis, or treatment recommendations. The Joe Tippens Protocol has not been validated in human clinical trials and is not endorsed by any medical organization or regulatory agency.

No compound described on this page is FDA-approved for cancer treatment (except mebendazole for parasitic infections). The protocol is based on one viral anecdote and preclinical (cell culture and animal) research that has not been replicated in controlled human studies.

Cancer is a life-threatening disease that requires professional medical treatment. Never replace or delay conventional cancer treatment based on information from this or any website. Always consult a qualified oncologist before making treatment decisions.

Dosages listed reflect community-shared protocols and are NOT medical recommendations. Individual responses vary. Many of these compounds carry significant risks including liver damage, drug interactions, and toxicity.

If you are currently undergoing cancer treatment, discuss any supplements or additional compounds with your oncology team before use.

The Joe Tippens Protocol

Want the Complete Protocol Guide?

How It Started

Joe Tippens — The Viral Anecdote

8 Compounds in the Protocol

Fenbendazole

Mebendazole

Ivermectin

Vitamin B17 / Amygdalin

FECO (Full Extract Cannabis Oil)

Methylene Blue

TUDCA

Activated Charcoal

How Key Compounds Work (Preclinical Data)

Fenbendazole — Triple Mechanism (Dogra 2018)

Mebendazole — Shared Benzimidazole Pathways

Ivermectin — Preclinical Anticancer Signals

Methylene Blue — Mitochondrial Targeting

Research Evidence by Compound

Safety & Risk Assessment

Community Protocol Variants

Key Study References

Key Takeaways

✅ What We Know

⚠️ What We Don’t Know

Related Products

Bacteriostatic Water

Sharps Container

TUDCA Supplement

Activated Charcoal

Curcumin Supplement

Deep-Dive Into Each Compound

💊 Fenbendazole Guide

🔬 Mebendazole Guide

🔵 Methylene Blue Guide

⬛ Activated Charcoal Guide

🌿 FECO Guide

⚗️ Vitamin B17 Guide

🛡️ TUDCA Guide

⚠️ Important Disclaimer