Ethyl eicosapentaenoic acid

Ethyl eicosapentaenoic acid
Identifiers
CAS number 86227-47-6 Y
PubChem 9831415
Jmol-3D images Image 1
Properties
Molecular formula C22H34O2
Molar mass 330.5 g mol−1
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Except where noted otherwise, data are given for materials in their standard state (at 25 °C, 100 kPa)
Infobox references

Ethyl eicosapentaenoic acid (E-EPA) is a highly purified, vacuum distilled derivate of the omega-3 fatty acid eicosapentaenoic acid (EPA). In Japan E-EPA is often called EPA-E.

Only EPA is considered to exihibit antipsychotic and antidepressive effects.[1] E-EPA is a psychotropic omega-3 fatty acid[2] and it is therefore of special interest in psychiatry.

Contents

Cardiovascular diseases, diabetes

The Japan Eicosapentaenoic acid (EPA) Lipid Intervention Study (JELIS) tested the effects of long-term use of E-EPA (1800 mg/day) in addition to a statin in Japanese patients with hypercholesterolemia. The results suggest that the addition of E-EPA to statin therapy prevents major coronary events, angina pectoris and clinical myocardial infarctions, apparently through mechanisms independent from regulation of the lipid metabolism. It has been suggested that the cardioprotective action of E-EPA is probably mediated by its anti-inflammatory properties.[3][4][5][6][7][8][9] In addition, E-EPA may improve the clinical outcome in type 2 diabetes [10][11][12][13] and its cardiovascular complications, such as coronary artery disease [14] and thickening of carotid arteries.[15] E-EPA may on the one hand reduce the platelet-derived microparticles (PDMP) and on the other enhance the cardioprotective hormone adiponectin in hyperlipidemic, diabetic patients.[16] According to Japanese mice studies, E-EPA may prevent and correct non-alcoholic fatty liver.[17][18]

Mental health

Acute psychosis

As adjuct therapy, E-EPA has been tested in first-episode psychosis.[19][20][21] The daily dosage of E-EPA given in these trials, i.e., 2 gram per day, corresponds to 10 to 15 helpings of Atlantic salmon.

In schizophrenia, the trials are based on the so-called membrane theory of the disease.[22][23][24][25][26][27][28][29] According to the Omega-3 Subcommittee of the American Psychiatric Association (APA), the evidence of the effects is still too weak to recommend the use of E-EPA,[30] but more studies are currently in progress.[31]

Clinical depression

Omega-3 fatty acids have been investigated as adjunct therapy for depression as they are anti-inflammatory agents and chronic low-grade inflammation has been linked to the disease.[32][33][34][35] Moreover, omega-3 content in the cell membranes of depressive persons is often decreased, and supplementation with omega-3 may correct this deficiency and improve the clinical outcome.[36][37][38][39][40][41] This hypothesis has been tested in a number of clinical trials using E-EPA, mostly 1 gram daily.[42]

Most (but not all) trials have yielded positive results.[43] In one study E-EPA boosted the effect of an antidepressive drug, fluoxetine.[44] According to a new report from Massachusetts General Hospital in Boston, E-EPA seems to be more effective than placebo as monotherapy in major depressive disorder.[45]

Bipolar depression

The first placebo-controlled study with ethyl esterized fish oil was carried out at Harvard University by professor Andrew L. Stoll, published in 1999.[46] His team later demonstrated that rigid cell mebranes in test subjects were smoothed by omega-3 fatty acids.[47] Subsequent studies at London's King's College Institute of Psychiatry have demonstrated the efficacy of E-EPA in bipolar patients.[48] One of the biochemical mechanisms seem to be enhancement of an amino acid called N-acetyl aspartate (NAA) in the brain.[49] E-EPA seems to exert similar effect on the NAA concentration as lithium which has been used for bipolar depression for decades.

Borderline personality disorder

So far one small clinical trial conducted on women has been published yielding promising results.[50]

Psychological stress

Animal tests demonstrate that E-EPA balances the metabolism of glucocorticoids (cortisol and cortisone) and may thus alleviate stress symptoms[51][52] and attenuate interleukine 1-beta (IL-1b) induced changes in dopamine and it's metabolites in the shell of the Nucleus accumbens.[52][53] The fatty acid EPA may confer neuroprotection in the amyloid-ß challenged aged hippocampus.[54][55]

Other conditions

E-EPA has been tested and found beneficial in anorexia nervosa,[56][57] hepatitis C,[58] in children with ulcerative colitis,[59] nonalcoholic fatty liver (steatohepatisis)[60] in psychological stress in postmenopausal middle-aged women,[61] and in women suffering from menopausal hot flushes.[62]

Safety aspects

E-EPA 2 g/day is generally well tolerated. Clinicians should be aware of possible increases in bleeding time, as well as changes in weight and lipid metabolism.[63]

References

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