Fat, Food, and Mood: Beyond Omega-3s

Publication
Article
Psychiatric TimesVol 33 No 12
Volume 33
Issue 12

Potential benefits and benign safety profile of omega-3s indicate a promising intervention.

TABLE. Dietary fat sources and psychiatric relevance

TABLE. Dietary fat sources and psychiatric relevance

SIGNIFICANCE FOR THE PRACTICING PSYCHIATRIST

SIGNIFICANCE FOR THE PRACTICING PSYCHIATRIST

Different sources of omega-3 and omega-6 fatty acids

Figure.

Over the past several decades, omega-3 polyunsaturated fatty acids (PUFAs) have been investigated as a potential therapy for psychiatric disorders. Supplementation has been found to ameliorate depressive symptoms, with particular advantage to those who are concurrently taking antidepressants. Benefits have also been found for bipolar depression, anxiety associated with substance dependence, ADHD symptoms, adverse effects of antipsychotics, and symptoms of schizophrenia and other neuropsychiatric disorders.1

However, clinical implementation of omega-3 recommendations has been complicated by inconclusive findings. Outcomes may be attenuated by considerable heterogeneity in research participants, study designs, and small sample sizes. While the evidence has not generated prescriptive guidelines for physicians, the potential benefits and benign safety profile indicate a promising intervention.

CASE VIGNETTE

L is a 47-year-old divorced woman with a history of MDD who reports the recurrence of depressed mood at a follow-up visit. She is taking sertraline (200 mg daily), which led to remission of her last depressive episode a year ago. She has low energy, amotivation, and poor concentration. Her appetite is “up and down” with a 15-lb weight gain in the past year; her BMI is 32. She is currently less depressed than previously but reports low mood. She sleeps 7 to 8 hours a night but rarely feels well rested; she uses CPAP for obstructive sleep apnea as instructed. She denies recent stressors or safety concerns, and further review for psychiatric symptoms is negative.

A review of her daily activity and diet reveals that she wakes around 7:30 am and eats a sausage and egg sandwich on her way to work. She is usually hungry by 10 am and has a doughnut from the break room. She frequently eats fast food for lunch (sometimes she orders a salad) and drinks a jumbo diet soda to maintain alertness throughout the afternoon. She often picks up a pizza or a hot sandwich after work or heats up a TV dinner at home. She reports having little energy or time to exercise. She wonders if the sertraline is no longer working and whether she should change medications.

 

What are healthy fats and why should psychiatrists care?

Previous clinical trials have not adequately considered omega-3s as a part of the larger dietary picture. Omega-3 PUFAs, along with omega-6 PUFAs, are essential nutrients that must be consumed in the diet. Alpha-linolenic acid, found in nuts and plant oils, is the essential omega-3 that can be converted to eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA), which have been the focus of most clinical studies in psychiatry. However, the conversion rate is low and genetically variable. Therefore, maintenance of EPA and DHA sufficiency may require direct dietary intake as supplementation (eg, fish oil) or from eating fatty cold-water fish (Figure).

EPA and DHA contribute to cardiovascular, inflammatory, and neurochemical functions and have an FDA-approved indication to lower triglycerides. Linoleic acid is the essential omega-6 and comprises approximately 8% of the caloric intake of the Western diet.2 It is converted to bioactive molecules involved in energy homeostasis, endothelial function, adaptive inflammation, and endocannabinoid neurochemistry.

The dietary balance between omega-3 and omega-6 intake is important because they have several counterbalancing physiological effects. A large epidemiological study concluded that lower intake of dietary PUFAs is significantly associated with all-cause mortality-linoleic acid showed the largest effect size.3 Clearly, omega-3s are not the whole story, and interactions with the broader dietary background must be considered to explain the equivocal nature of the literature.

A few other classes of fatty acids warrant mention (Table). Monounsaturated fatty acids (MUFAs), which include oleic acid from olive oil, are another major dietary fat with health benefits. They have not been the focus of the psychiatric literature, but they are considered heart healthy and likely to benefit brain function. On the unhealthy list are the saturated and trans-fatty acids. Both are associated with increases in all-cause mortality, and it is recommended to limit intake, especially of trans fats.3

Finally, of interest to the bigger picture of evaluating dietary fats in psychiatric illness is an older literature that describes associations between low cholesterol and suicide. Early literature suggested increased rates of suicide and violent behavior in patients treated with cholesterol-lowering medications, and mechanisms that link cholesterol to suicidal behavior have been proposed.4,5 These studies were not consistently replicated in subsequent trials, and recent reviews show this hypothesis remains unresolved.6 Regardless of the current inability to draw conclusions, it provides additional support for the link between fat metabolism and mood control.

Therefore, general dietary advice to eat less fat, which has been promoted to the American public for decades, is not sufficient guidance and is potentially problematic for psychiatric and other health measures. The type of fat matters!

Omega-3s in psychiatric research

There is ongoing debate about how EPA and DHA benefit psychiatric disorders. EPA seems to play a greater role in endothelial function, including the vascular systems, and has oxidation products with anti-inflammatory effects.7 DHA is enriched in cell membranes, especially in neuronal tissue, and affects membrane signaling kinetics and neuronal function.8 While cell membrane DHA concentrations differ consistently between patients with MDD and controls, there has been no significant improvement with DHA mono-supplementation.1 However, the most up-to-date and standardized meta-analysis found that the beneficial effect of a combination of EPA and DHA on depression (standardized mean difference of 0.398) was similar to that reported in meta-analyses of antidepressants.9,10

A meta-analysis of combination therapies using antidepressants and adjunctive omega-3 supplementation found an effect size of 0.61.11 Both reviews revealed an effect of EPA independent of DHA that suggests the benefit may be mediated through anti-inflammatory effects rather than correction of a deficit of membrane DHA. This makes theoretical sense given preclinical studies that associate systemic inflammation with fatigue, anhedonia, anorexia, sleep disturbance, and decreased synthesis of central monoamines.12

Further support for this hypothesis comes from the observation that the benefit from EPA monotherapy for MDD patients depended on increased pretreatment biomarkers of inflammation; EPA was less effective than placebo or DHA in subjects with low inflammation.13 In this study, obese patients were more likely to have a higher number of elevated inflammatory biomarkers and experienced the most improvement on the Hamilton Depression Rating Scale (HAM-D) in response to EPA. This may explain some of the variation in outcomes between studies, which have not always accounted for inflammatory status.

 

Omega-6s in psychiatric research

Omega-6 PUFAs are less studied in psychiatry; however, there is a vast and controversial literature regarding other health effects, particular on cardiovascular disease and cancer. Since the Western diet has increased from approximately 2% to 8% of total energy from linoleic acid over the past century, its health consequences (or benefits) have been questioned.2 There are 2 camps of thought:

1. The increase in linoleic acid intake underlies increased inflammation, which increases risk of disease.

2. The increase in linoleic acid intake is associated with reduced rates of heart disease and all-cause mortality.

Theoretical biochemistry supports the first, since linoleic acid is the precursor for arachidonic acid, which in turn is the direct precursor for inflammatory eicosanoids. However, there is a lack of data to support increases in arachidonic acid or inflammation following increased dietary linoleic acid intake. In fact, there are data to support decreases in inflammation with increased dietary linoleic acid intake.14 As with omega-3 research, broader dietary patterns have not been considered for many of the reports that describe effects of dietary linoleic acid, which may partially explain the variability.

The few studies of linoleic acid intake in psychiatric patients are also inconclusive. A longitudinal study found dietary linoleic acid intake was associated with an increased risk of depression in men, but not in women.15 However, other studies found plasma linoleic acid (and other PUFAs and MUFAs) associated with improved depression scores.16 Plasma linoleic acid levels may also be negatively associated with HAM-D scores in older persons (aged 60 to 86 years) with a prior episode of major depression.17 In individuals with bipolar disorder, improved psychiatric outcomes were associated with higher dietary linoleic acid intake and plasma levels.18-20 Despite the relative paucity of studies that have directly evaluated omega-6s in mood disorders, we know that arachidonic acid is crucial in brain development and is an important PUFA in neuronal membranes.

Back to the clinic: putting research into practice

At this time, there is not sufficient evidence to generate specific guidelines for PUFA supplementation for different mental health conditions. Given the evidence summarized above, it is appropriate to recommend intake of enough fish oil so that the total EPA dose is at least 1 g daily (typically 2 or 3 capsules). This will include DHA at nonspecific doses. While studies attempt to identify the active ingredient in omega-3 supplementation, it has not been shown that purified monotherapy outperforms the combination.

In 2006, the American Psychiatric Association adopted the consensus recommendations of the American Heart Association for psychiatric patients with mood, impulse, or psychotic disorders. The recommendations include consumption of fish at least twice weekly and supplementation of 1 to 9 g daily of combined EPA and DHA.21 Patients who have higher levels of inflammation may be more likely to benefit from higher doses of omega-3 supplementation. The presence of inflammation can be inferred from past medical history and metabolic risk factors (eg, BMI, hyperlipidemia).

There are many adequate fish oils on the market, with the caveat that one should seek products with a seal of third-party testing to ensure purity and quality (ie, United States Pharmacopeia [USP]). Fish oils are usually well tolerated, with a low risk of serious adverse effects. Most commonly, people report a fishy aftertaste or mild nausea, which typically does not lead to discontinuation.22 Up to 5 g daily is considered safe for the general population, although in the US doses higher than 3 g daily require monitoring by a physician, because of the theoretical risk of bleeding.

Finally, it is important to remember that supplements do not justify an otherwise poor diet. We recommend talking to patients about their dietary patterns and helping them realize that diet may play a role in how they feel. Low-fat diets may be a relative contraindication for psychiatric patients, and supplementation with omega-3s may be beneficial; however, dietary supplements are not substitutes for healthy eating.

Disclosures:

Dr. Evans is Assistant Research Professor, Department of Psychiatry, University of Michigan, Ann Arbor, MI. Dr. Edwards is a fourth-year psychiatry resident at the University of Michigan, Ann Arbor. The authors report no conflicts of interest concerning the subject matter of this article.

References:

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2. Blasbalg TL, Hibbeln JR, Ramsden CE, et al. Changes in consumption of omega-3 and omega-6 fatty acids in the United States during the 20th century. Am J Clin Nutr. 2011;93:950-962.

3. Wang DD, Li Y, Chiuve SE, et al. Association of specific dietary fats with total and cause-specific mortality. JAMA Intern Med. 2016;176:1134-1145.

4. Muldoon MF, Rossouw JE, Manuck SB, et al. Low or lowered cholesterol and risk of death from suicide and trauma. Metabolism. 1993;42:45-56.

5. Cantarelli Mda G, Tramontina AC, Leite MC, Goncalves CA. Potential neurochemical links between cholesterol and suicidal behavior. Psychiatry Res. 2014;220:745-751.

6. While A, Keen L. The effects of statins on mood: a review of the literature. Eur J Cardiovasc Nurs. 2012; 11:85-96.

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9. Mocking RJ, Harmsen I, Assies J, et al. Meta-analysis and meta-regression of omega-3 polyunsaturated fatty acid supplementation for major depressive disorder. Transl Psychiatry. 2016;6:e756.

10. Schalkwijk S, Undurraga J, Tondo L, Baldessarini RJ. Declining efficacy in controlled trials of antidepressants: effects of placebo dropout. Int J Neuropsychopharmacol. 2014;17:1343-1352.

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12. Capuron L, Miller AH. Immune system to brain signaling: neuropsychopharmacological implications. Pharmacol Ther. 2011;130:226-238.

13. Rapaport MH, Nierenberg AA, Schettler PJ, et al. Inflammation as a predictive biomarker for response to omega-3 fatty acids in major depressive disorder: a proof-of-concept study. Mol Psychiatry. 2016;21:71-79.

14. Bjermo H, Iggman D, Kullberg J, et al. Effects of n-6 PUFAs compare d with SFAs on liver fat, lipoproteins, and inflammation in abdominal obesity: a randomized controlled trial. Am J Clin Nutr. 2012;95: 1003-1012.

15. Wolfe AR, Ogbonna EM, Lim S, et al. Dietary linoleic and oleic fatty acids in relation to severe depressed mood: 10 years follow-up of a national cohort. Prog Neuropsychopharmacol Biol Psychiatry. 2009;33:972-977.

16. Panagiotakos DB, Mamplekou E, Pitsavos C, et al. Fatty acids intake and depressive symptomatology in a Greek sample: an epidemiological analysis. J Am Coll Nutr. 2010;29:586-594.

17. Jadoon A, Chiu CC, McDermott L, et al. Associations of polyunsaturated fatty acids with residual depression or anxiety in older people with major depression. J Affect Disord. 2012;136:918-925.

18. Evans SJ, Assari S, Harrington GJ, et al. Plasma linoleic acid partially mediates the association of bipolar disorder on self-reported mental health scales. J Psych Res. 2015;68:61-67.

19. Evans SJ, Kamali M, Prossin AR, et al. Association of plasma omega-3 and omega-6 lipids with burden of disease measures in bipolar subjects. J Psych Res. 2012;46:1435-1441.

20. Evans SJ, Prossin AR, Harrington GJ, et al. Fats and factors: lipid profiles associate with personality factors and suicidal history in bipolar subjects. PloS One. 2012;7:e29297.

21. Freeman MP, Hibbeln JR, Wisner KL, et al. Omega-3 fatty acids: evidence basis for treatment and future research in psychiatry. J Clin Psychiatry. 2006;67:1954-1967.

22. Freeman MP, Fava M, Lake J, et al. Complementary and alternative medicine in major depressive disorder: the American Psychiatric Association Task Force report. J Clin Psychiatry. 2010;71:669-681.

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