PEA Osteo Research

​Palmitoylethanolamide Osteoarthritis

​Palmitoylethanolamide Diseases / By /

Studies/Abstracts:  Palmitoylethanolamide and Osteoarthritis

“Palmitoylethanolamide shows benefit in knee osteoarthritis

    • Steels E & al.
    •  Inflammopharmacology   29 Mar 2019
  • Palmitoylethanolamide (PEA) improved function and reduced pain, stiffness, and anxiety without serious toxicity in a randomized controlled trial (RCT) of patients with knee osteoarthritis (KOA).

Why this matters

  • PEA has the potential to be a natural, nontoxic, and targeted treatment option for KOA.

Study design

  • RCT of 111 patients with mild to moderate knee osteoarthritis, receiving 300 mg PEA, 600 mg PEA, or placebo daily for 8 weeks.
  • Function was assessed by the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC).
  • Funding: None disclosed.

Key results

  • Efficacy at week 8, with each PEA dose compared with placebo:
    • Reduction in WOMAC total score: 300 mg, P=.037; 600 mg, P=.001.
    • Reduction in WOMAC pain subscore: 300 mg, P=.007; 600 mg, P<.001.>
    • Reduction in WOMAC stiffness subscore: 300 mg. P=.049; 600 mg, P=.001.
    • Reduction in WOMAC function subscore: 300 mg, NS; 600 mg, P=.003.
    • Reduction in anxiety on the Depression Anxiety Stress Scale: 300 mg, P=.042; 600 mg, P=.043.
  • Safety at week 8, with each PEA dose compared with placebo:
    • No differences in erythrocyte sedimentation rate (ESR) and C-reactive protein (CRP).
    • No differences in numerous biochemical and hematological parameters.
    • No reports of serious toxicity.

Limitations

  • No reporting of nonserious adverse events.
  • Single-center study.”

https://www.univadis.co.uk/viewarticle/palmitoylethanolamide-shows-benefit-in-knee-osteoarthritis-664187

. 2017; 13: 229.
Published online 2017 Aug 2. doi: 10.1186/s12917-017-1151-z
PMCID: PMC5541643
PMID: 28768536

A novel composite formulation of palmitoylethanolamide and quercetin decreases inflammation and relieves pain in inflammatory and osteoarthritic pain models

Domenico Britti,1 Rosalia Crupi,2 Daniela Impellizzeri,2 Enrico Gugliandolo,2 Roberta Fusco,2 Carlo Schievano,3 Valeria Maria Morittu,1 Maurizio Evangelista,4 Rosanna Di Paola,2 and Salvatore Cuzzocreacorresponding author2,5
Author information Article notes Copyright and License information Disclaimer
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5541643/

Abstract

Background

Osteoarthritis (OA) is a common progressive joint disease in dogs and cats. The goal of OA treatment is to reduce inflammation, minimize pain, and maintain joint function. Currently, non-steroidal anti-inflammatory drugs (e.g., meloxicam) are the cornerstone of treatment for OA pain, but side effects with long-term use pose important challenges to veterinary practitioners when dealing with OA pain. Palmitoylethanolamide (PEA) is a naturally-occurring fatty acid amide, locally produced on demand by tissues in response to stress. PEA endogenous levels change during inflammatory and painful conditions, including OA, i.e., they are typically increased during acute conditions and decreased in chronic inflammation. Systemic treatment with PEA has anti-inflammatory and pain-relieving effects in several disorders, yet data are lacking in OA. Here we tested a new composite, i.e., PEA co-ultramicronized with the natural antioxidant quercetin (PEA-Q), administered orally in two different rat models of inflammatory and OA pain, namely carrageenan paw oedema and sodium monoiodoacetate (MIA)-induced OA. Oral treatment with meloxicam was used as benchmark.

Conclusion

The present findings shed new light on some of the inflammatory and nociceptive pathways and mediators targeted by PEA-Q and confirm its anti-inflammatory and pain-relieving effects in rodent OA pain models. The translatability of these observations to canine and feline OA pain is currently under investigation.

Conclusions

PEA-Q is a novel co-ultramicronized formulation of PEA and quercetin whose effects were investigated in two pre-clinical models of OA pain in rats. Oral administration of PEA-Q decreased pain sensitivity, improved locomotor function, reduced inflammatory signs and mediators and lowered histological damage score. Although the underlying mechanism(s) of the observed effects are beyond the scope of our study, the particular cellular targets of PEA (e.g., mast cells and microglia) [], redundancy of its receptors (direct and direct agonism on nuclear and membrane cannabinoid receptors) [] and oxidative stress addressed by quercetin [] comprise targets that could be different from standard pharmacological tools (i.e., NSAIDs). Importantly, toxicological studies show that micronized and ultramicronized PEA is safe, the LD50 being greater than 2000 mg/kg []. Individually or in association with different antioxidant polyphenols, micronized and ultramicronized PEA has a long track record of use in human and veterinary patients, with good-to-excellent tolerability []. Moreover, prolonged use of PEA is not associated with the development of tolerance []. There is an unmet need in veterinary medicine for the development of new agents to treat OA-associated pain which target alternative mechanisms distinct from currently approved drugs. The collective observations presented here propose that PEA-Q shows promise for multimodal pain management in canine and feline OA.”

Full Study:  https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5541643/

 

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