Two antiparasitic drugs have ended up at the center of an online conversation about cancer. One is approved for humans, one is not. Here's an honest look at what the science says, what it doesn't say, and why both drugs deserve more rigorous study than they've gotten.
This article is educational. It does not recommend, prescribe, or sell any medication. Neither ivermectin nor fenbendazole is FDA-approved as a cancer treatment. Do not start, stop, or change any medical treatment based on what you read here. Talk to a qualified oncologist about any decisions related to cancer care.
In 2016, a man named Joe Tippens was diagnosed with small-cell lung cancer that had spread throughout his body. His prognosis was poor. He was also enrolled in a clinical trial of an experimental immunotherapy called pembrolizumab (Keytruda). On the advice of a veterinarian, he began taking a canine dewormer — fenbendazole — alongside the trial drug. Months later, his scans showed no evidence of cancer.
Tippens attributed his remission to fenbendazole. His story spread on social media, and a large online community of people self-administering veterinary antiparasitics for cancer grew up around it. Around the same time, a parallel conversation emerged about ivermectin — another antiparasitic drug — based on a growing body of laboratory research suggesting possible anticancer activity.
The story is compelling. It's also scientifically complicated. Tippens was on an immunotherapy drug at the time of his remission that has, on its own, produced dramatic responses in a subset of patients with his type of cancer. Isolating the effect of one variable when two are changing at once is exactly what clinical trials are designed to do, and exactly what has not happened here.
Ivermectin was developed in the 1970s from a compound produced by the soil bacterium Streptomyces avermitilis. Its discovery was recognized with the 2015 Nobel Prize in Physiology or Medicine. It has been used safely in hundreds of millions of doses worldwide, primarily to treat parasitic diseases like river blindness (onchocerciasis) and intestinal threadworm (strongyloidiasis), both of which are FDA-approved indications in the United States. Topical ivermectin is also approved for rosacea and head lice.
At the doses used for these approved indications, ivermectin has a well-characterized safety profile. It is on the World Health Organization's list of essential medicines.
In the last decade, researchers have published a growing number of preclinical studies — meaning studies in cell cultures and animal models, not in humans — suggesting ivermectin may have effects on cancer-related pathways. Proposed mechanisms include inducing programmed cell death in certain tumor cell lines, interfering with the Wnt/β-catenin signaling pathway, disrupting mitochondrial function, and affecting cancer stem cell populations.
These findings are scientifically interesting. They are not the same thing as evidence that ivermectin treats cancer in people. Many compounds look promising in a dish and fail in humans, for reasons that include poor bioavailability, different pharmacokinetics, off-target effects at the doses required, and the sheer biological complexity of a tumor growing in a living person.
As of this writing, ivermectin is not approved by the FDA or any other major regulator as a cancer treatment. It is also not approved for the prevention or treatment of COVID-19, a separate controversy that the FDA, WHO, and multiple large randomized trials have addressed directly.
Fenbendazole is a benzimidazole antiparasitic used widely in veterinary medicine — for dogs, cattle, sheep, goats, horses, and laboratory rodents. It has never been approved for human use by the FDA or the European Medicines Agency. It belongs to a broader chemical family that includes two drugs that are approved for humans: mebendazole and albendazole, both used to treat intestinal parasites.
Fenbendazole's mechanism is to bind to a protein called β-tubulin, which disrupts microtubule assembly inside parasite cells. Microtubules are also essential to cell division in human cells, which is why several well-established chemotherapy drugs — the taxanes (paclitaxel, docetaxel) and the vinca alkaloids (vincristine, vinblastine) — work by targeting microtubules, though through different binding sites and mechanisms. This mechanistic overlap is part of what drew researchers to the question of whether fenbendazole might have anticancer activity.
Laboratory studies have reported that fenbendazole can:
These are real findings from real peer-reviewed studies. They are also early-stage findings, many at drug concentrations that may not be achievable in human blood, and some of which have not been consistently reproduced.
Cutting against them is a 2008 Stanford study, published in Cancer Research, that specifically set out to test whether fenbendazole affected tumor growth in rodent models. The authors concluded that their data did not support further testing of fenbendazole as a cancer therapy — though they left open the possibility that related benzimidazole compounds might be worth exploring. This is a reminder that the preclinical picture is mixed, not unanimous.
There have been no randomized controlled clinical trials of fenbendazole in humans for any cancer indication. What exists in the medical literature is a small number of case reports — published descriptions of individual patients who self-administered the drug, with varied outcomes. Some describe tumor regression. At least two describe drug-induced liver injury that resolved when the drug was discontinued. Reviews of anecdotal reports compiled from online communities describe hundreds of stories, but these lack the controls, follow-up, and verification that would let researchers draw conclusions.
"Clinical trials play a central role in medicine and cancer research. In the case of fenbendazole, there is no proven benefit but several potential risks." — American Cancer Society
It is worth acknowledging something the skeptical coverage sometimes glosses over: the reason no large human trials exist is not that researchers have tested fenbendazole in humans and found it ineffective. It's that the economic structure of drug development rewards patented, expensive molecules, and fenbendazole is an off-patent veterinary generic with no commercial sponsor. Multiple researchers and bioethicists have argued that this is a problem — that promising cheap drugs get stranded in scientific limbo because no one stands to profit from proving them out. A related compound, oxfendazole (a major metabolite of fenbendazole), has recently received FDA fast-track designation for developing it as a treatment for human trichuriasis, which is an interesting indicator that the regulatory path for benzimidazoles in humans is not closed.
But "more study is warranted" is not the same as "this drug treats cancer." Both statements can be true at once, and it's important to hold them separately.
People who self-administer veterinary fenbendazole for cancer are taking on several risks that rarely make it into the online testimonials:
None of this is a moral judgment of patients who have tried it. For someone facing a grim prognosis, the calculus looks different than it does from the outside, and the impulse to try something — anything — is deeply human. The point is just that the risks are real and deserve to sit on the same page as the hopeful stories.
Three things appear to be simultaneously true:
The reasonable response to all three is the same: well-designed human clinical trials, run by independent researchers, with proper controls and endpoints. Several early-stage trials of benzimidazoles in oncology are in various stages of planning or recruitment. Until those generate results, the honest answer to "does fenbendazole cure cancer?" is "we don't know, and the people telling you they do know — in either direction — are going beyond what the evidence supports."
A few things worth doing:
Disclaimer. This article is provided for general educational and informational purposes only. It is not medical advice, not a recommendation to use any medication, and not a substitute for consultation with a qualified healthcare professional. Neither ivermectin nor fenbendazole is approved by the U.S. Food and Drug Administration for the treatment or prevention of cancer. Fenbendazole is not approved for any human use. The author and publisher make no claims that any substance discussed here treats, cures, prevents, or diagnoses any disease. If you are a patient considering any change to your medical care, please discuss it with your oncologist or primary care provider.
Sources consulted include the American Cancer Society, the U.S. Food and Drug Administration, peer-reviewed reviews published in Anticancer Research and Cancer Research, the Centers for Disease Control and Prevention, and the World Health Organization. Full references available on request.
