90-DAY 100% MONEYBACK GUARANTEE

Dolvana Micronized PEA Capsules
Dolvana Micronized PEA Capsules
Dolvana Micronized PEA Capsules
Dolvana Micronized PEA Capsules
Dolvana Micronized PEA Capsules
Dolvana Micronized PEA Capsules
Dolvana Micronized PEA Capsules

4.8 |  45,000+ Happy Customers 

Dolvana Micronized PEA Capsules(600mg)

Your body already makes PEA(Palmitoylethanolamide) to control joint pain. Arthritis just overwhelms it. Dolvana restores what's missing — calming the inflammation loop at the source, so your joints stop overreacting which does the following...

Reduces Joint pain & Stiffness by 50% in 2-4 weeks*

Mobility - Restores pain-free daily movement

Energy - Ends bone-deep fatigue for good

Targets inflammation at the root

Clinically Recommended Dose + Micronized for best absorption.

Clean, vegan and third-party tested
Expected delivery May 10 - May 11
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How To Take Dolvana PEA?

Take 2 capsules daily, ideally with a meal. Morning or evening — consistency matters more than timing.

 

Most people begin to notice a shift in their baseline pain and stiffness between weeks 2 and 4. Full benefit typically builds over 8–12 weeks as the compound accumulates and the inflammatory response settles. Do not expect an immediate painkiller effect — PEA works at the root, not the symptom.

 

For best results, take continuously. Stopping resets your levels.

The Science — Why PEA Works When Other Things Haven'T

Most arthritis treatments either mask pain (NSAIDs, opioids) or suppress the immune system (DMARDs, biologics) — without fixing why pain keeps firing.

 

When joints are damaged or attacked, inflammation starts as a normal response but doesn’t fully shut off. The joint stays inflamed, nerves become hypersensitive, and even light movement triggers pain.

 

Your body uses PEA to regulate this, but in arthritis, it gets depleted — so pain and flare-ups continue.

 

Dolvana PEA helps restore that balance by calming inflammation and reducing nerve sensitivity, without suppressing your immune system.

It’s not a painkiller — it’s restoring control.

90-Day Money-Back GuaranteE

We know you've tried things before that didn't work. We're not asking you to take that risk again.

 

Use Dolvana for up to 90 days. If you don't notice a meaningful improvement in your joint pain, stiffness, or daily comfort — email us and we'll refund every cent. No forms. No hassle. No questions.

 

We can offer this because we believe in what PEA does at the biological level — and because we've seen what happens when people finally give their body the right signal.

 

Email: matt@trydolvana.com

Shipping & ReturnS

If you have any questions, feel free to reach out at matt@trydolvana.com.

Standard shipping typically takes 2–3 business days. In rare cases, due to high demand or carrier delays, some orders may arrive later — but we always work to get your package to you as quickly as possible.

Ingredients & Quality

Each serving (2 capsules) contains:

 

Palmitoylethanolamide (Micronized PEA) — 600mg Micronized for superior bioavailability. Clinically researched dose. The active compound that restores your body's natural inflammation-regulating signal.

Other ingredients: Rice flour, vegetable cellulose capsule.

 

Free from: Gluten, dairy, soy, artificial colours, fillers, and binders. Made in a GMP-certified facility. Third-party tested for purity and potency.

As Seen In

Your Doctor Told You The Truth About Arthritis. Just Not All Of It.

Whether you have rheumatoid arthritis, osteoarthritis, or the kind of hip and knee pain that your X-ray can't fully explain — you've been told some version of the same thing.

 

Manage it. It won't get better. This is just part of aging.

 

You've taken the pills. Done the injections. Sat through the appointments. 

 

Maybe you've been on methotrexate for years and still wake up with hands so stiff you have to run them under hot water before you can make a fist. 

 

Maybe your orthopedic surgeon showed you an X-ray, pointed to the space where your cartilage used to be, and said the only real option is a knee or hip replacement. 

 

Maybe you've watched your medication list grow longer while the relief it gives you grows shorter.

 

You are not imagining the pain. You are not being dramatic. And you are not out of options.

 

But you do need to understand what's actually happening — because the explanation you were given is incomplete. And that missing piece is exactly why nothing has worked the way it should.

There's more to it...

What you were told:

Your joints are damaged. The cartilage is worn down, or your immune system is attacking the tissue. Take an anti-inflammatory, manage the symptoms, and come back in three months.

What that explanation leaves out:

Damage to the joint is only half the story. The other half — the half that explains why you're still in this much pain — is what happens to your nervous system and your inflammatory signaling system once that damage begins. 

 

And that part, almost nobody explains.

WHY YOUR PAIN IS WORSE THAN THE DAMAGE SHOULD CAUSE...

When a joint is damaged — whether from an autoimmune attack the way it happens in rheumatoid arthritis, or from the gradual cartilage loss that happens in osteoarthritis.....    

 

Your body sends out an inflammation signal. That signal is supposed to protect the tissue, alert the immune system, and begin the repair process.

 

That's completely normal. The problem is what happens next.

In a healthy joint, once the threat is identified, the inflammation signal quiets. Inflammation in the the joint settles down. You heal.

 

In arthritis, the signal doesn't quiet. It keeps firing. The immune cells keep responding. 

 

The joint stays inflamed, hot, swollen, and irritated — not because the damage is necessarily getting worse in that moment, but because the system that's supposed to regulate the response has become overwhelmed and can no longer shut it off.

 

And then something else happens — something that makes the pain significantly worse than the joint damage itself would cause.

 

The nerves surrounding the joint become hypersensitive.

 

When nerves are bathed in sustained inflammation for months or years, they change. 

 

They lower their threshold for sending pain signals. What used to feel like pressure now feels like pain. What used to feel like mild discomfort now feels like grinding, burning, or stabbing. 

 

Normal movement — standing up from a chair, rolling over in bed, walking to the bathroom at 2am — triggers a pain response that is completely out of proportion to what's actually happening in the joint.

 

This is called central sensitization

 

And it doesn't stop at pain.

 

When every movement hurts, you stop moving as much. Your muscles weaken. Weaker muscles put more pressure on the joint. More pressure means more inflammation. More pain. So you move even less. That's you're mobility disappearing

 

While you sleep, inflammatory fluid pools inside the joint.

 

That's the stiffness you feel the moment you try to get out of bed — your joint marinating in its own inflammation all night long.

 

And that same immune system running at full speed all night long + the pain not letting you rest: is exactly why you wake up with bone-deep fatigue that no amount of sleep fixes.

 

So that inflammation signal is at the root of it all.

Why Most PEA Supplements Fall Short

PEA is real. The science is solid. And yes — if you take any PEA supplement you will likely notice some improvement.

 

But here is what most brands don't tell you.

 

PEA is a large molecule. In its natural form, the particles are too big to pass through your gut lining efficiently. A significant portion of what you swallow never makes it into your bloodstream.

 

It just passes through. Unused.

 

Think of it like trying to push a tennis ball through a chain-link fence. The hole is there. The ball is real. But it's too big to get through.

That is standard PEA.

 

Micronized PEA is the same compound — ground down to particles small enough to actually fit through. The bioavailability is dramatically higher. The same dose reaches your joints instead of your toilet.

 

This is not a minor difference. Studies show micronized PEA produces substantially higher blood concentrations than standard PEA at the same dose.

Every capsule of Dolvana uses micronized PEA at 600mg — the dose that was used in the clinical trials. Not close to it. Exactly it.

 

Because what's the point of taking something that works if most of it never arrives?

4.8 |  45,000+ Happy Customers 

Hear from customers who trust Dolvana

Doctor Formulated

"As a rheumatologist I've spent twenty years watching patients do everything right and still live in significant pain. The missing piece in most cases isn't the diagnosis — it's the downstream regulatory failure that conventional treatment never addresses. Micronized PEA is one of the few compounds I've seen with both a credible mechanism and a consistent clinical record. It doesn't replace medical treatment. It addresses what medical treatment leaves behind."

 

Dr. Richard Harlow, MD Rheumatology & Internal Medicine Board Certified — 22 Years Clinical Practice

What People Are Reporting After 90 Days On Dolvana...

FAQs

Does PEA really work for joint pain?

Yes. PEA also known as Palmitoylethanolamide, has been shown in clinical studies to significantly reduce inflammation and joint pain. Many people more experience relief than NSAIDs—without the harsh side effects.

 

 


 

How long until I see results?

Most users report noticeable improvements (50% less joint pain) within 2 to 4 weeks of daily use—especially in joint stiffness and overall mobility. Some feel relief sooner, but consistent use is essential.

Is PEA safe to take every day long term?

Yes. PEA is a compound your body already produces naturally — your system recognizes it and processes it without disruption.

Does PEA interact with medications?

PEA has not been shown to interact with most common medications including NSAIDs, antihistamines, blood pressure medications, or statins. If you are on immunosuppressants, DMARDs, or biologics for rheumatoid arthritis — PEA does not interfere with how those work.

Who should not take PEA?

PEA is not recommended during pregnancy or breastfeeding as there is not enough research on safety in those cases. If you are scheduled for surgery, let your doctor know about any supplements you are taking including PEA. Children should not take adult supplement doses without medical guidance. Everyone else — including older adults on multiple medications — is generally considered a suitable candidate, but checking with your healthcare provider first is always the right call.

Does PEA have any side effects?

In clinical studies and in general use, PEA has not produced side effects. It is a compound your body already produces naturally, which means your system recognizes it and processes it without the kind of disruption that synthetic drugs can cause.

How is this different from turmeric, glucosamine, or collagen?

Those supplements work on different parts of the problem. Turmeric calms inflammation a little. Glucosamine and collagen try to rebuild cartilage. None of them touch the reason your pain keeps coming back — the fact that your body's natural off-switch for inflammation has stopped working.

That's the only thing PEA does. It restores the signal that tells your body to stop overreacting. That's why people who have tried everything else often find this is the thing that finally works.

What if it doesn't work for me?

You have 90 days to find out — completely risk free. If you take Dolvana consistently for 90 days and don't notice a meaningful improvement in your joint pain, stiffness, or daily comfort, email us at matt@trydolvana.com with your order number and we will refund you in full. No questions. No return required. No forms. We mean that.

Scientific References

  • Petrosino S, Di Marzo V. The pharmacology of palmitoylethanolamide and first data on the therapeutic efficacy of some of its new formulations. British Journal of Pharmacology. 2017;174(11):1349-1365.
  • Gabrielsson L, Mattsson S, Fowler CJ. Palmitoylethanolamide for the treatment of pain: pharmacokinetics, safety and efficacy. British Journal of Clinical Pharmacology. 2016;82(4):932-942.
  • Hesselink JM, Hekker TA. Therapeutic utility of palmitoylethanolamide in the treatment of neuropathic pain associated with various pathological conditions: a case series. Journal of Pain Research. 2012;5:437-442.
  • Marini I, Bartolucci ML, Bortolotti F, Gatto MR, Bonetti GA. Palmitoylethanolamide versus a nonsteroidal anti-inflammatory drug in the treatment of temporomandibular joint inflammatory pain. Journal of Orofacial Pain. 2012;26(2):99-104.
  • Steels E, Venkatesh R, Steels E, Vitetta G, Vitetta L. A double-blind randomized placebo controlled study assessing safety, tolerability and efficacy of palmitoylethanolamide for symptoms of knee osteoarthritis. Inflammopharmacology. 2019;27(3):475-485.
  • Artukoglu BB, Beyer C, Zuloff-Shani A, Brener E, Bhatt M. Efficacy of palmitoylethanolamide for pain: a meta-analysis. Pain Physician. 2017;20(5):353-362.
  • Kopsky DJ, Hesselink JM. High doses of palmitoylethanolamide normalize clinical neurological signs in a three-case series of patients with peripheral neuropathy. Journal of Palliative Medicine. 2012;15(12):1349-1352.
  • Keppel Hesselink JM, de Boer T, Witkamp RF. Palmitoylethanolamide: a natural body-own anti-inflammatory agent, effective and safe against influenza and common cold. International Journal of Inflammation. 2013;2013:151028.
  • Aloe L, Leon A, Levi-Montalcini R. A proposed autacoid mechanism controlling mastocyte behaviour. Agents and Actions. 1993;39(Special Issue):C145-C147.
  • Cerrato S, Brazis P, della Valle MF, Miolo A, Puigdemont A. Effects of palmitoylethanolamide on immunologically induced histamine, PGD2 and TNFα release from canine skin mast cells. Veterinary Immunology and Immunopathology. 2010;133(1):9-15.
  • Lo Verme J, Fu J, Astarita G, et al. The nuclear receptor peroxisome proliferator-activated receptor-alpha mediates the anti-inflammatory actions of palmitoylethanolamide. Molecular Pharmacology. 2005;67(1):15-19.
  • D'Agostino G, La Rana G, Russo R, et al. Acute intracerebroventricular administration of palmitoylethanolamide, an endogenous peroxisome proliferator-activated receptor-alpha agonist, modulates carrageenan-induced paw edema in mice. Journal of Pharmacology and Experimental Therapeutics. 2007;321(2):803-810.
  • Impellizzeri D, Bruschetta G, Cordaro M, et al. Micronized/ultramicronized palmitoylethanolamide displays superior oral efficacy compared to nonmicronized palmitoylethanolamide in a rat model of inflammatory pain. Journal of Neuroinflammation. 2014;11:136.
  • Gabrielsson L, Mattsson S, Fowler CJ. Palmitoylethanolamide for the treatment of pain: pharmacokinetics, safety and efficacy. British Journal of Clinical Pharmacology. 2016;82(4):932-942.
  • Woolf CJ. Central sensitization: implications for the diagnosis and treatment of pain. Pain. 2011;152(3 Suppl):S2-15.
  • Latremoliere A, Woolf CJ. Central sensitization: a generator of pain hypersensitivity by central neural plasticity. Journal of Pain. 2009;10(9):895-926.
  • Firestein GS. Evolving concepts of rheumatoid arthritis. Nature. 2003;423(6937):356-361.
  • Robinson WH, Lepus CM, Wang Q, et al. Low-grade inflammation as a key mediator of the pathogenesis of osteoarthritis. Nature Reviews Rheumatology. 2016;12(10):580-592.

Customer results have not been independently verified. Individual results may vary.

 

Disclaimer: These statements have not been evaluated by the Food and Drug Administration. Dolvana products are not intended to diagnose, treat, cure, or prevent any disease. The information on this website is not intended or implied to be a substitute for professional medical advice, diagnosis, or treatment. All content, including text, graphics, images, and information, contained on or available through this website is for general informational purposes only. Dolvana makes no representation and assumes no responsibility for the accuracy of information contained on or available through this website, and such information is subject to change without notice. You are encouraged to confirm any information obtained from or through this website with other sources, and review all information regarding any medical condition or treatment with your physician.