Same here.

Thanks. It will be encouraging if you are able to produce UA efficiently that way. I could not determine that I was so I switched to 1,000 mg UA/day. I’m not sure about the expectations time line for VO2max change but the changes in my lower body muscular performance – back to a more youthful profile – took the full period of several months noted in the research. Initial cellular changes can be noted around six weeks as I recall.

I purchased their capsules once early on and they sent me a third-party purity analysis. Of course, this does not certify that the capsules contain the full amount. They seemed legit.

thank you ive decided to extend my experiment to 4 months based on your info. And also because I’m now craving pomegranate!

I’m taking these cravings as a positive sign that I’m “metabotype A” (able to convert all the punicalagins into urolithin -a)

If you pattern is similar to mine, the change will catch you by surprise at an exercise session. Initially, you may write it off as just having a good day but it will persist.

The Timing Reality Check: Urolithin A Rescues Aging Brain Biology, But Fails to Reverse Established Memory Loss

Urolithin A (UA) is a widely discussed postbiotic molecule known for triggering mitophagy—the cellular recycling of damaged mitochondria. While previous studies tout its benefits in Alzheimer’s models and muscle health, its efficacy in natural brain aging has remained uncertain. This new research investigates a critical clinical question: Does the timing of mitophagy activation matter for cognitive preservation?

The short answer is yes. The researchers found that while UA effectively prevents age-related cognitive decline when administered early, it fundamentally fails to reverse memory loss once significant mitochondrial and synaptic damage has already occurred.

The study employed two complementary mouse models to test early versus late intervention. For the late-stage model, 16-month-old naturally aging C57BL/6J mice—which already exhibit cognitive deficits—were given UA for eight weeks. On a molecular level, the compound performed precisely as intended. It boosted ATP production, enhanced mitochondrial fusion proteins (Mfn1 and Mfn2), upregulated biogenesis markers like PGC-1a and Nrf2, and cleared pathological tau proteins (PHF-1) from hippocampal synapses. Yet, despite this impressive molecular repair, the mice showed no improvement in spatial or recognition memory. The biochemical rescue did not translate into functional cognitive recovery.

Conversely, the early intervention model utilized 5-month-old SAMP8 mice, a strain that undergoes accelerated aging and typically develops cognitive deficits by six months. When these mice received UA prior to the onset of memory loss, the results were striking. Hippocampal ATP levels surged by over 4-fold, toxic tau accumulation was blocked, and spatial learning was significantly preserved. Intriguingly, after this successful cellular stabilization, markers for mitophagy and biogenesis actually downregulated, suggesting the mitochondrial pool had reached a healthy homeostatic state that no longer required aggressive turnover.

These findings establish a critical reality check: metabolic therapies and mitophagy activators are not magic erasers for established neurodegeneration. Once synaptic networks are compromised, fixing the cellular power grid is insufficient. Compounds like UA must be utilized preventatively to protect brain healthspan.

Context:

• Paper: Early mitophagy activation by Urolithin A prevents, but late activation does not reverse, age-related cognitive impairment
• Researchers: This research was conducted by scientists at the Laboratory of Neurobiology of Aging, Fundación Ciencia & Vida, and Universidad San Sebastián in Santiago, Chile.
• Journal: It is published in the journal npj Aging.
• Impact Evaluation: The impact score of this journal is 5.6, evaluated against a typical high-end range of 40–60+ for top general science, therefore this is a Medium impact journal.

FYI, this is not for UA but for NAD supplements: Wellness LabsRx was among the brands that listed “liposomal” but failed testing by SuppCo: SuppCo Testing Finds Widespread Failures in NAD+ Products - Nutraceuticals World

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Similarly, NOW tested berberine supplements and Wellness Labs Rx was among the worst ones: NOW Finds Quality Issues in Berberine Supplements On Amazon - Nutraceuticals World

18 of 33 brands tested contained less than 40% of labeled potency, and seven of the 33 tested samples had 1% or less of berberine potency. These seriously flawed brands were tested for the first time by NOW’s program, and may be new brands. These included Earth Bare, Greabby Gummies, GreenPeople Formula, KoNefancy, Satoomi, Vitamiscence, and Wellness Labs Rx.

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SuppCo also tested UA products: https://files.supp.co/tested/urolithin-a.pdf

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Wellness Labs Rx was not part of the tested products, but it shows the field is plagued by fraud.

fwiw here’s the company’s president (and the only person publicly associated with the company): https://www.linkedin.com/in/rose-cabasso-b635661a0/

It seems the current company behind the brand (Health and Wellness Associates, Inc) was incorporated in 2023, even though the brand existed before (probably under a different company?). Rose Cabasso also owns MyLiquidNaturals.

If the above is correct, then Wellness Labs Rx is a very low-quality brand that should be avoided at all costs.

By the way, just published: First Reported Human Cases of Urolithin A Renal Calculi 2026

In more recent times, ULA has been proposed as an antiaging compound, leading to the growing use of both diet and supplements to raise blood levels.2 Here we present a series of urinary stones containing urolithin A, the first such, to our knowledge, reported in humans.
Over-the-counter supplements were reviewed with these 6 patients, and none were taking ULA supplements.
Though stones derived from drugs or supplements are rare, their recognition by stone analysis is important so the causative exposure can be stopped. Health fads and drug development may expose people to poorly soluble compounds that crystallize in the urinary tract. Stone analysis laboratories must be vigilant to recognize and identify new stone components.
ULA supplements have been well tolerated in human studies, though trials have been short-term (up to 4 months). Only 1 urinary stone event was reported, without stone composition details.
This inability to produce potentially-therapeutic ULA from foods in some patients has prompted the development of commercially-available ULA supplements. These supplements bypass microbial conversion and provide significantly higher systemic exposure—plasma and urine ULA levels can be up to 6 times greater than those from dietary sources.9 Nonetheless, none of our ULA stone formers reported ULA supplement use. We anticipate cases may emerge as supplement use increases, given the uniformly high ULA excretion it induces.
ULA, a compound derived from the gut microbiome metabolism of food polyphenols and also sold as an over-the-counter health supplement, can precipitate from urine and be incorporated into urinary stones. Addition of ULA as a standard in IR spectral libraries of stone analysis laboratories is critical to allow ULA identification so clinicians can intervene and identify foodstuffs or supplements that are contributing to stone formation.

I’m not sure it’s relevant unless someone has a history of calcium oxalate/phosphate stones, low urine volume, or hyperoxaluria?

One thing I find interesting that most people ignore is that the solubility of various ions varies by the pH of the solute. (normally urine). I have studied this with gout because it is obvious that a low urinary pH plus low urine volume makes gout more likely.

There are stones eg (Ca-P) which are more likely at higher urinary pH. Hence it is not a one way issue, but there seems to be good evidence that alkaline urine (and oddly enough acidic fecal matter) are both good for healthspan.

Thank you for this. Depressing news but the price was likely the hint.

It is interesting that UA is being positioned as a geroprotective. I have viewed it as a modulator of other functions that support primary geroprotectives, such as vigorous exercise in old age. I take UA to address a specific muscle problem that appears to be genetic. Going back as far as 1986, my LDH levels have ranged from borderline to clinically low and my genetic profile suggests a predominance of endurance muscles. This combination appears to have proved beneficial in the competitive distance running I engaged in for most of my adult life. Subjectively, my muscles are very slow to “warm up” but quite literally, the longer i ran – up to many hours – the stronger they became. This profile shifted in my mid-70’s when it became clear that I was unable to push my lower body muscles sufficiently on hill climbs to reach Zone 5 periodically, one of my goals. The limitation profile was definitely muscular and not CV. UA has definitely reversed much (maybe 70%) of this problem and I am again able to push my muscles hard enough to move into an anerobic zone with high respiration and heartbeat. I am aware of the nuance in summarizing these issues as briefly as I have, my only point here is to present an example in which UA has resulted in muscle performance gain.

You’re welcome. Btw, I first googled the brand and couldn’t find much, then asked ChatGPT to dig deeper and was surprised it found all those things. Good to know to do a background check on other companies.

To be fair and give them a chance, I wrote an email to the company. We’ll see it they come back with anything substantive or just a third-party certificate of purity that tells you nothing about capsule dose.

Let us know how it goes.

Rodent study finds life extension with a urolithin A mix: SRN-901, a Novel Longevity Drug, Extends Lifespan and Healthspan by Targeting Multiple Aging Pathways

Put off by the cost of Urolithin A, I’ve been taking its sister molecule Urolithin B for a month. Everychem sells two grams of powder for about $30. Beyond it’s lower cost, however, the B metabolite has been shown to improve kidney function, exerting anti-fibrotic and anti-inflammatory effects in rats with induced kidney damage. This is what attracted my interest.

A blood test yesterday showed that my GFR has increased from 28 to 34, a rise of 20% in 30 days. This increase may not be due entirely to Urolithin B. During the same period, I’ve been taking 2 tsp/day of sodium citrate, an extremely effective acid neutralizer. I also can’t rule out a possible delayed response to SS-31, which I tried two months ago.

That’s likely to be the citrate. I would be careful to balance out cations, however.

Balance with what?

As for the GFR result, it may well be the citrate. Also a more alkaline diet. With kidney disease, acid is the enemy. Acidosis is a killer.

And at the very least, the blood test I had, a Comprehensive Metabolic Panel, showed that Urolithin B hasn’t been detrimental.

Have you considered pomegranate peel extract?
Assuming you’re the right Metabotype It should get you to an effective dose of urolithin a very cheaply (3g of powder im a bit of kefir).

You can test for Urolithin A - to see if its working - and that’s only a one time test. Or yiu can take my approach - if you start by dosing alongside actual pomegranate: if you find yourself craving pomegranate it’s a decent sign you’ve got the right gur bacteria.

Thanks for the suggestion. I’ll try it.

You are taking Sodium, balancing with Potassium and Magnesium is a good idea, Calcium can help, but at the moment I go for NaKMg.

I sell this in the UK