Background

The purpose of this review is to examine the effect of Omega-3 Fatty acids on mortality, morbidity, and adverse events in patients with acute myocardial infarction (AMI).

Methods

Data Sources: MEDLINE, EMBASE, and the Cochrane Library through May 2018. Study Selection: Randomized Controlled trials (RCT). Certainty of evidence was assessed with the GRADE system. Interventions: omega 3 fatty acids against placebo or no treatment. Primary and secondary outcomes: All-cause death, cardiovascular death, new AMI, stroke, need for therapeutic angioplasty or By-pass, new diagnosis of cancer and incidence of adverse events.

Results

For the efficacy endpoints we included 10 RCT (24,414 patients). Omega 3 fatty acids probably make little or no difference to all-cause mortality (4 studies 9141 patients RR 1.06 - CI95% 0.90 to 1.27, moderate certainty), cardiovascular mortality (3 studies 4304 patients RR 0.93 - CI95% 0.63 to 1.37, moderate certainty), new AMI (RR 1.24 CI95% 0.71 to 2.14 - moderate certainty), any cardiovascular event (RR 0.95 95%CI 0.86 to 1.05; low certainty due to risk of bias and imprecision), and stroke (RR 1.2 95%CCI 0,66–2,19 - moderate certainty). Regarding adverse events, we are uncertain if Omega 3 fatty acids improve/reduce non severe adverse events (RR 1.39 95% CI 0.36 to 5.34; very low certainty). There is probably little or no difference in the outcome suspension due to adverse events (RR 1.19 CI 95% 0.97 to 1.47; moderate certainty).

Conclusions

For adult patients with AMI, omega 3 fatty-acids probably yield no benefit to patient important outcomes.

Electronic supplementary material

The online version of this article (10.1186/s12872-019-1086-3) contains supplementary material, which is available to authorized users.

Keywords: Omega 3 fatty acid, Polyunsaturated fatty acids, Myocardial infarction, Secondary prevention, Systematic review

Search strategy and elegibility criteria

We searched for randomized controlled trials comparing omega 3 fatty acids against placebo or no treatment in the following literature databases, regardless of publication status and without language restrictions: the Cochrane Central Register of Controlled Trials from the Cochrane Library, MEDLINE, EMBASE, Epistemonikos and LILACS from inception until May 2018.Details of the full search strategies are provided in the Additional file1: Appendix 2. Our gray-literature search included searches in Grey Matters Tool [8]. We also searched the Canadian Agency for Drugs and Technology in Health, Google Scholar, Trip Database, National Institute for Health and Care Excellence, McMaster University, McMaster Health Forum, PROSPERO,ClinicalTrials.gov, and manually examined the reference lists of all reviews identified.

As for the inclusion criteria, we included RCTs of adults that suffered a myocardial infarction (according to the study’s definition) and were randomized to receive omega 3-fatty acid supplementation at doses greater than or equal to 400 mg daily versus placebo/No treatment. The treatment should have started within 6 weeks after the initial diagnosis of the myocardial infarction. We considered any mode of administration of the intervention, such as dietary supplementation (fish oils, soya bean oils, seeds, refined EPA, DHA, ALA) or, oil or capsule form or as foodstuffs. To be eligible, studies had to report at least one of the following outcomes: All-cause death, cardiovascular death, new acute myocardial infarction, stroke, need for therapeutic angioplasty or By-pass, new diagnosis of cancer and incidence of adverse events.

Study selection and data extraction

Two investigators (G.B. and F.P.) independently reviewed the titles and abstracts identified and full texts of included articles in order to determine eligibility using the EROS tool for systematic reviews early phases [9]. Disagreements or uncertainties were resolved by consensus of the whole team with an additional investigator (A.I.). We accepted the primary authors’ definition of AMI, stroke, adverse event and serious adverse event.

The risk of bias was assessed independently by two reviewers on an outcome by outcome basis using a modification of the Cochrane Risk of Bias Tool which considers, sequence generation, allocation concealment, blinding, number of patients with missing outcome data, selective outcome reporting, and other sources of bias [10]. We used the Grading of Recommendations Assessment, Development and Evaluation system to assess the certainty of the effect (also known as quality of evidence or confidence in evidence) for each outcome and for the entire body of evidence [11,12]. Certainty of the effect takes into consideration the study design (in this case, randomized clinical trials); risk of bias, precision, consistency, directness of the evidence; and the probability of publication bias [13].

Statistical analysis

We analyzed the data using Review Manager, version 5.3 (Cochrane Collaboration). We used random-effects models for all analyses (Mantel–Haenszel risk ratios [RRs] for dichotomous outcomes) since significant heterogeneity was expected. Publication bias was assessed through visual inspection of funnel plots (Additional file1: Appendix 3) and the subjective impression of the reviewers (G.B., F.P. and A.I.) considering the size of the included studies and sponsorship. We also contacted investigators to consult whether they had knowledge of other potentially relevant unpublished trials.

We used Cochrane’s test for heterogeneity to determine whether studies in a meta-analysis evaluated the same underlying sizes of effect. We used the I² statistic to test the degree of heterogeneity among studies (the proportion of total observed variability due to genuine variation rather than random error within studies) [14].

We planned a priori the following subgroup analyses as possible explanations for heterogeneity: 1) type of fatty acid: eicosapentaenoic acid and docosahexaenoic acid versus alpha-linolenic acids with a postulated larger effect for the latter [9,15]; 2) Dose effect: high dose (consumption of more than 4.5 g daily) of Omega 3 fatty acids could be associated with a larger treatment benefit; 3) Type of omega 3: synthetic omega 3 (in comparison with dietary recommendations with increased omega 3 fatty acid intake) could be associated with a larger treatment benefit; 4) Risk of bias: Studies with high risk of bias could be associated with a larger treatment benefit. We visually analyzed the results of each subgroup comparison and additionally tested for interaction by using a chi-square significance test [14].

Dealing with missing data

For the primary analysis we used a complete case-analysis approach, i.e. we excluded participants considered to have missing data. For those outcomes in which a clinically significant effect was observed (Relative risk CI95% not including 1), we performed a sensitivity analysis to challenge the possibility of risk of bias due to missing data following the approach described by Guyatt et.al [16,17] (complete description of the implemented sensitivity analysis is available in Additional file1: Appendix 4).

Patient and public involvement

Patients were not involved in this review.

Study characteristics

We identified 610 potentially relevant records. After screening titles, abstracts and full texts we included 11 publications for quantitative analysis (Fig. 1.).

The characteristics of the 11 RCTs included are summarized in Table 1. In six [18–23] of them the intervention was implemented in the form of dietary recommendations while EDH-EPA (synthetic form of omega 3 fatty acids) was implemented in the remaining four [24–28].

Risk-of-Bias assessment

In five of the included studies [18,22,25–28], patients, investigators and outcome assessors were blinded. Four of those studies were judged as low risk of bias as no additional methodological issues were noted. Regarding the remaining studies, six were judged as to carry moderate or high risk of bias (Fig. 2). Although one of the included studies had no apparent methodological limitations, we decided to judge it as high risk of bias [27] because the author was accused of misconduct and data fabrication in two different trials in which he was involved [30,31]. We assumed the trials to have important lost to follow-up when the authors did not offer enough information to analyze the impact of missing data or if the performed sensitivity analysis significantly altered the effect estimate or the confidence interval for each outcome. (Additional file1: Appendix 4).

All-cause mortality

All the included trials addressed this outcome. Omega 3 fatty acids reduced the risk of all-cause mortality (RR 0.86, CI 95% 0.72 to 1.02). Considering the basal risk (risk without the intervention) as themean of the risk in the control groups of the included RCT, the mortality reduction was 1.4% (CI95% 2.5 to 0) at a mean follow up of 3 years. We judged the certainty in the estimates of effect as low due to risk of bias, imprecision and inconsistency (I² 85%) (Fig. 3), (Table 2).

Cardiovascular mortality

Nine of the included trials addressed this outcome. Omega 3 fatty acids reduced the risk of cardiovascular mortality (RR 0.77, CI 95% 0.65 to 0.91). Considering the basal risk as themean of the risk in the control groups of the included RCT, the cardiovascular mortality reduction was 1.5% (CI95% 2.3 to 0.6) at a mean follow up of approximately 3 years. We judged the certainty in the estimates of effect as low due to risk of bias and inconsistency (Fig. 4), (Table2).

Acute myocardial infarction

Seven of the included trials addressed this outcome. Omega 3 fatty acids reduced the risk of Myocardial infarction (RR 0.77, CI 95% 0.6 to 0.99). Considering the basal risk as themean of the risk in the control groups of the included RCT, the cardiovascular mortality reduction was 2.2% (CI95% 3.8 to 0.1) at a mean follow up of approximately 3 years. We judged the certainty in the estimates of effect as low due to risk of bias, imprecision and inconsistency) (Fig. 5), (Table2).

Stroke

Five of the included trials addressed this outcome. Omega 3 fatty acids did not reduce the risk of stroke (RR 1.2, CI 95% 0.66 to 2.19). Considering the basal risk as themean of the risk in the control groups of the included RCT a marginal increase in the risk of stroke was observed RD 0.2% (CI95% -0.4 to 1.4%) at a mean follow up of approximately 3 years. We judged the certainty in the estimates of effect as moderate due to imprecision (Fig. 6), (Table2).

Need to therapeutic revascularization

Three of the included trials addressed this outcome. Omega 3 fatty acids did not reduce the risk of therapeutic revascularization (RR 1.0 CI 95% 0.91). Considering the basal risk as themean of the risk in the control groups of the included RCT no differences in the need of therapeutic revascularization were observed RD 0% (CI95% -1.9 to 2.4%) at a mean follow up of approximately 3 years. We judged the certainty in the estimates of effect as moderate due to imprecision (Fig. 7), (Table2).

Treatment suspension due to adverse events

Two of the included trials addressed this outcome. Omega 3 fatty acids increased the relative risk of treatment suspension due to adverse effects (RR 1.19 CI 95% 0.97 to 1.47). Considering the basal risk as themean of the risk in the control groups of the included RCT no differences in the risk of treatment suspension due to adverse effects was observed RD 0.3% (CI95% -0.1 to 0.7%) at a mean follow up of approximately 3 years. We judged the certainty in the estimates of effect as moderate due to imprecision (Fig. 8), (Table2).

Cancer

Two of the included trials addressed this outcome. Omega 3 fatty acids increased the relative risk of cancer (RR 1.25 CI 95% 0.94 to 1.66). Considering the basal risk as themean of the risk in the control groups of the included RCT only a marginal increase in cancer occurrence was observed RD 0.3% (CI95% -0.1 to 0.7%) at a mean follow up of approximately 3 years. We judged the certainty in the estimates of effect as very low due to imprecision and indirectness (Fig. 9). The results are shown in a Summary of Finding Table (Table2).

Subgroup analysis

Inconsistency was observed for overall mortality, cardiovascular mortality and myocardial infarction outcomes. In performing the prespecified risk of bias subgroup analysis we observed that the benefits (mortality, cardiovascular mortality and MI reduction), suggested by the overall pooled results, were not present when pooling the subgroup of studies in which the intervention was applied in a blinded fashion (low risk of bias). Although the test for subgroup differences was only statistically significant for overall mortality (p < 0.05) visual inspection of the forest plots suggest a similar subgroup effect for the three outcomes. The Fatty acid type subgroup analysis also showed a possible differential effect (less cardiovascular mortality) when EPA-DHA was implemented in comparison to ALA (RR 0.66, IC95% 0.35–1.27 for ALA vs. RR 0.82, IC95% 0.72–094) for EPA + DHA. No significant differences were observed when different doses were used.

We then decided to include, in the summary of findings tables, both the results of the overall pooled estimates and the results of the blinded trials pooled estimates (Table2). We used primarily a 4 mg threshold to evaluate the effect of the dose of omega 3 fatty acid which showed no effect on the evaluated outcomes. A secondary analysis using a 1 mg threshold showed also no impact on those outcomes.

Strengths and limitations of this study

• The present systematic review provides estimations regarding the efficacy of supplemental omega 3 fatty acids in the context of myocardial infarction secondary prevention paying special attention to the risk of bias of the included studies

• Unlike most of the published reviews we focused in the population of patients that had suffered an acute myocardial infarction

• It provides the most comprehensive and trustworthy body of evidence up to date, including studies not included in any other published reviews [19,20,22,23,28].

• We performed a thorough analysis of the information and identified significant differences in the results of the primary studies that could be explained by methodological limitations in some of them.

Funding

The group recieved no external funding. Publication fees were funded by Hugo Norberto Catalano, Ariel Izcovich, Federico Popoff and Giselle Balaciano.

Availability of data and materials

Not applicable.

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Supplementary Materials

Data Availability Statement

Not applicable.