Tonight, if there's a "tongkat ali + Fadogia" bottle in your cart, take the Fadogia half out. There are zero human studies on it and the only animal research shows testicle, liver, and kidney damage.
That's the general answer. Your stack is different.
Check your whole stackThe viral testosterone herb with podcast fame and zero human trials.
SkipTonight, if there's a "tongkat ali + Fadogia" bottle in your cart, take the Fadogia half out.
There are zero human studies on Fadogia agrestis, and the only animal research shows the same doses that raised testosterone also damaged the testes, liver, and kidneys. You keep the half with actual evidence (tongkat ali) and drop the untested one.
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The Verdict
Fadogia agrestis is a shrub from West Africa, traditionally used as an aphrodisiac. It went viral as a natural testosterone booster after a popular health podcast featured it.
A viral testosterone booster with zero human studies, and the rat studies show organ damage.
In rats, something in the plant's stem nudged testosterone up. But the same doses also damaged the testes, liver, and kidneys, like a tool that does the job and breaks the machine at the same time. And nobody has ever tested whether either half of that happens in people.
Nobody, on current evidence. No human study shows it helps anyone.
You want higher testosterone, better libido, or more muscle, and especially if you want to stay fertile.
Want the full evidence? Keep scrolling
There isn't one. Because there are no human trials, there is no evidence-based dose, timing, or form. The figures you'll see online (commonly 300 to 1200 mg/day of stem powder or loosely-labelled extract) come from consumer convention and guesswork scaled up from rat experiments, not from any study in people.
| Population | Dose | Form | Evidence |
|---|---|---|---|
| General adult | No evidence-based dose | Stem powder / extract | No human trial |
| Men seeking higher testosterone | No evidence-based dose | "Standardised" extract | No human trial |
| Older adults (50+) | No evidence-based dose | — | No human trial |
Absorption tips: none can be given. With no human pharmacokinetic study, how well your body absorbs it, how long it lasts, and whether food matters are all unknown.
This is the part with the most actual content, and it's a warning, not a green light. There is no human safety data. The only safety information that exists comes from the same rat studies used to claim a benefit, and it points the wrong way.
In rats, higher doses impaired testicular function and changed liver and kidney markers, at doses overlapping with the ones that raised testosterone. Human relevance is untested, but it is the only toxicology that exists.
Adding an unproven steroidogenic agent on top of TRT, hCG, or a stack is completely uncharacterised. Avoid.
Given the rodent liver and kidney signal, combining with anything that taxes those organs is a theoretical added load. No human data exists to reassure you.
Upper limit: none established. No regulator (EFSA, the FDA, or the NIH Office of Dietary Supplements) has evaluated Fadogia agrestis, set a safe limit, or issued a monograph. It's sold as an unregulated botanical.
And that "low" is generous. It reflects a real rat safety signal, not any proven human benefit. For raising testosterone in people, the honest rating is "no evidence at all".
Go Deeper
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Join The Verdict — freeFadogia agrestis is sold as a natural testosterone and libido booster, usually as the headline ingredient or the partner in a "tongkat ali + Fadogia" stack. The pitch is that this West African shrub raises testosterone, increases sex drive, and improves erections, with the implication that it supports muscle, energy, and "vitality" like a mild hormone therapy. Most of its fame came from being mentioned on a hugely popular health podcast, after which sales and searches spiked.
The marketing leans on two things: a traditional-use story (used as an aphrodisiac in parts of West Africa) and a "studies show it boosts testosterone" claim. The traditional-use story is real. The "studies show" claim is where it falls apart, because the studies are in rats, not people.
To be fair: there genuinely is a rat literature showing a testosterone response, and the compound isn't invented. The problem is what was found, in what species, and what came with it.
| Claim | Strength | Reality |
|---|---|---|
| Raises testosterone (humans) | NONE | Zero human trials. The claim is rat data in a human costume. |
| Boosts libido (humans) | NONE | Zero human trials. Rat sexual-behaviour data does not transfer. |
| Improves erections (humans) | NONE | Only a rat ED model exists (PMID 35969364), not a human study. |
| Builds muscle / body composition | NONE | Never studied for this in any species. |
| Raises testosterone (rats) | WEAK | Real in rats, but non-transferable and coupled to organ toxicity. |
| Safe for humans | NO DATA | No human safety data. Adverse rat signal in testes, liver, kidneys. |
What would change this: an independent, blinded, placebo-controlled human trial measuring testosterone by mass spectrometry with a built-in organ-safety panel. None exists.
The honest answer: nobody has shown how it works in humans, because nobody has tested it in humans. In rats, aqueous extract of the stem has been linked to higher testosterone and more sexual behaviour. The usual explanation is that something in the plant stimulates the hormonal axis that drives testosterone, or acts directly on the testosterone-making cells in the testes.
Here's the practical catch. No single compound has been isolated and confirmed as the active ingredient. If you don't know which compound does the work, you can't standardise a product around it. A bottle that says "standardised 20:1 extract" is telling you about a manufacturing ratio, not a verified active dose, because there's no validated marker to standardise against.
Everything in this section is rat biology. Rodent testosterone responses have a long history of failing to repeat in men, which is exactly why "it raised testosterone in rats" is a starting hypothesis, not a result you can act on.
The conflict here isn't between human trials. It's inside the rat literature, where the same extract points two ways at once.
Current direction: the evidence hasn't moved in years. It remains a small rat literature with no human follow-up, which is the strongest possible signal that this should be treated as unproven.
Lab: rats given measured doses over a few days. Reality: people taking unmeasured capsules for months. When you take it, you're not reproducing a study, you're running an untested experiment on yourself.
With no validated active compound, "standardised" means nothing you can check, and adulteration or contamination would go unnoticed. The rat toxicity signal makes that uncertainty consequential, not academic.
Testosterone rose and organs were damaged at overlapping rat doses. You can't keep the marketing claim and discard the toxicity, because they came from the same animals at the same doses.
If low testosterone is the real concern, the levers with actual evidence are sleep, alcohol, training load, and eating enough. In active, under-fuelled men, low testosterone is usually downstream of under-eating and over-training, and the fix is restoring energy and recovery, not an unproven herb. If symptoms are real, that warrants a clinician and a blood test, not a botanical with a rat toxicity signal.
Food-first note: not applicable. This isn't a nutrient, and there's no deficiency to correct.
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