The potential benefit of marine n-3 PUFA on CHD has been extensively examined in both observational studies and clinical trials, with the majority of studies favouring a beneficial effect of n-3 PUFA( Reference He, Song and Daviglus 1 – Reference Saravanan, Davidson and Schmidt 4 ).
Thus, several prospective cohort studies have reported an inverse relationship between fish consumption and CHD( Reference He, Song and Daviglus 1 , Reference Lemaitre, King and Mozaffarian 5 – Reference Yuan, Ross and Gao 14 ). However, other studies have not supported these findings( Reference Amiano, Machón and Dorronsoro 15 , Reference Ascherio, Rimm and Stampfer 16 ). Most epidemiological studies have evaluated the dietary intake of fish using questionnaires, but relatively few of these studies have differentiated between different types of fish and their content of marine n-3 PUFA. In this study, we evaluated fish intake using detailed and validated FFQ, allowing us to differentiate between consumption of fatty and lean fish, and additionally to calculate the intake of total and individual marine n-3 PUFA.
Large secondary prevention trials have been performed evaluating dietary interventions with fish servings or supplementation with fish oil capsules. Although earlier trials such as the diet and reinfarction trial( Reference Burr, Fehily and Gilbert 17 ), Gruppo Italiano per lo Studio della Sopravvivenza nell'Infarto Miocardico (GISSI) Prevenzione( 18 ) and Japan EPA Lipid Intervention Study trials( Reference Saito, Yokoyama and Origasa 19 ) have demonstrated a reduction in CHD events following consumption of marine n-3 PUFA, more recent trials have not supported these findings( Reference Kromhout, Giltay and Geleijnse 20 – Reference Galan, Kesse-Guyot and Czernichow 22 ). Controversy therefore still remains regarding the potential benefits from fish consumption and n-3 PUFA supplements in the prevention of CHD, and guidelines are currently under review.
In this large Danish cohort study, including 3089 validated cases of incident myocardial infarction (MI), we investigated the association of fish consumption and dietary intake of marine n-3 PUFA with incident MI. The present study is one of the largest cohort studies on fish consumption and MI, and notably the study includes a relatively high number of female cases.
Methods
Study population and design
The Danish Diet, Cancer and Health study is a prospective cohort study, which has been described in detail previously( Reference Tjønneland, Olsen and Boll 23 ). In brief, 160 725 persons aged 50–64 years were invited between December 1993 and May 1997. Inclusion criteria were as follows: born in Denmark, living in the urban areas of Copenhagen and Aarhus and not registered with a cancer diagnosis in the Danish Cancer Registry at the time of invitation. A total of 57 053 persons accepted the invitation and were enrolled into the study. Participants registered with a previous MI or cardiac arrest were excluded. If a cancer diagnosis was reported, which was not already recorded in the Cancer Registry at the time of invitation, participants were excluded in line with the intention-to-include criteria. At baseline, each participant filled in a detailed questionnaire on diet, lifestyle, socio-economic status and medical history. Data from dietary questionnaires were analysed in a traditional cohort design including the entire cohort. Participants were followed-up until July 2013. The present study was conducted according to the Helsinki Declaration and approved by the regional Ethics Committees.
Dietary assessment
At baseline, participants filled in a detailed 192-point, semi-quantitative FFQ, including twenty-six specific questions regarding the intake of fish and food products containing fish. The questionnaire has been validated and described in detail previously( Reference Tjønneland, Overvad and Haraldsdóttir 24 ). In short, participants were asked to estimate their daily intake of foods in natural units such as pieces of fruits, slices of bread and glasses of different drinks. For mixed dishes and meals, sex-specific portion sizes were calculated using data from a calibration study. By multiplying the frequencies of intake by the portion size, the individual average intake in g/d of all foods and nutrients was calculated. Different species of fish were categorised as either lean or fatty depending on their content of n-3 PUFA, below or above 1 g/100 g, respectively. Fatty fish mainly comprised herring, salmon, trout and mackerel, whereas lean fish comprised mainly plaice, flounder and cod( Reference Joensen, Overvad and Dethlefsen 7 ).
The dietary intakes of specific nutrients including total and individual marine n-3 PUFA – EPA, docosapentaenoic acid (DPA) and DHA – were calculated using FoodCalc software (www.ibt.ku.dk/jesper/foodcalc) based on Danish Food Composition Tables.
Outcome assessment
We identified all participants in the cohort who were registered with an incident diagnosis of MI in the Danish National Patient Registry and/or the Danish Causes of Death Registry, according to the International Classification of Disease (ICD) 8 (410.00–410.99) or ICD-10 (I21.0–I21.9) coding, during the study period. Furthermore, all cases of cardiac arrest (ICD-8: 427.27 or ICD-10: I46.0–I46.9) were included if the arrest was considered to be of cardiac origin after validation in each individual case. The Danish National Patient Registry( Reference Andersen, Madsen and Jørgensen 25 ) contains information on diagnoses and interventional procedures in relation to all hospital ward admissions since 1977, whereas all visits to outpatient clinics and emergency rooms have been registered since 1995. The Danish Causes of Death Registry contains diagnoses for all deaths since 1943. Patients were registered in both registries in accordance with ICD-8 until 1 January 1995 and subsequently according to ICD-10. An earlier study from our Department validated the MI diagnosis from baseline through 2003 by complete review of all medical records, and found a positive predictive value >92 % when the diagnoses were obtained from a hospital ward( Reference Joensen, Jensen and Overvad 26 ). All validated cases of MI from the validation study were readily accepted as cases for the present study. From January 2004 through July 2013, all participants with an incident MI diagnosed from a ward were accepted as cases without further validation. All other diagnoses of incident MI and cardiac arrest were validated by reviewing a complete list of diagnoses and interventional procedures recorded in the Danish National Patient Registry for each potential case. Cases of incident MI were categorised as fatal or non-fatal depending on their vital status 28 d after the event. Vital status was obtained using the Civil Registration System.
Statistics
Exposure variables were categorised into quintiles based on the cohort distribution. A test for trend across quintiles was carried out. Furthermore, we also evaluated the exposure variables as continuous variables using restricted cubic splines with three knots.
Measures of association were assessed using Cox proportional hazards multivariate regression models with age as the time axis and delayed entry. Analyses were conducted separately for men and women. Participants were treated as at risk from baseline until either MI, death, emigration or end of follow-up occurred.
To address potential confounding, we adjusted for traditional risk factors of MI (model A2), including smoking habits (never, former or current (<15, 15–25, >25 g/d) smoker), BMI (kg/m2), waist circumference (cm), physical activity (h/week), alcohol intake (g/d), educational level (basic school, higher education: 1–3 or >3 years) and, for women, menopausal status (pre or postmenopausal). Second, we adjusted for either medical history (model B) or additional dietary covariates (model C) in separate models. Regarding medical history, we adjusted for history of diabetes mellitus (yes/no), hypertension (yes/no) or hypercholesterolaemia (yes/no), including participants on antihypertensive medications or lipid-lowering drug treatment, respectively. Adjustment for additional dietary variables depended on the exposure variable (details specified in the relevant tables). All continuous variables were included in the models as restricted cubic splines with five knots. Potential confounders were selected a priori based on current knowledge of risk factors for MI.
The proportional hazards assumption was checked by visual inspection of log–log plots and by evaluation of scaled Schoenfeld residuals, with no significant violations. Estimates with P values (two-tailed) <0·05 were considered statistically significant. STATA, version 13.1 (StataCorp. LP) was used for statistical analysis.
Results
The Diet, Cancer and Health cohort included a total of 57 053 participants. From these, an initial 1506 were excluded when baseline questionnaires were missing (n 42) or when participants were identified with a cancer diagnosis in the Danish National Patient Registry before baseline (n 564). We also excluded participants with previous MI or cardiac arrest before inclusion (n 900). In our study population, we identified 3089 cases of incident MI during a median follow-up time of 17·0 years. After case verification, we excluded subjects for whom information on one or more covariates used in the adjusted analyses was missing (n 643). Thus, 3028 cases were included in the final analyses (Fig. 1).
Baseline risk factors for CHD were generally more prevalent in cohort members who experienced a MI during follow-up (‘cases’) than in the cohort as a whole (Table 1). Accordingly, we observed a larger proportion of men, higher age, BMI and waist circumference, and a larger proportion of smokers among cases. In contrast, cases had lower weekly physical activity and lower educational level compared with the cohort. With regard to medical history, more cases suffered from hypertension, hypercholesterolaemia and diabetes mellitus. Consumption of fruits and vegetables was lower among cases, whereas we did not find any marked differences between cases and the cohort with regard to fish consumption and use of fish oil supplements. Baseline characteristics were also evaluated by the intake of fatty and lean fish for men and women separately, in order to describe potential confounders. Data are included in the online Supplementary Material (online Supplementary Table S1·2).
DPA, docosapentaenoic acid.
* Comparison of baseline characteristics for the cohort as a whole (including both cases and non-cases) and cases with myocardial infarction separately.
Fish consumption and incident myocardial infarction
The median intake of fatty fish was 15·1 and 12·2 g/d for men and women, respectively, whereas the median intake of lean fish was 24·4 and 21·0 g/d for men and women, respectively, with minor variations between cases and cohort (Table 1).
In Table 2, we present hazard ratios (HR) for the association between fish consumption and incident MI distributed by quintiles. For men, fatty fish intake was inversely associated with MI in the four higher quintiles compared with the lowest. The association was attenuated by adjustment for traditional risk factors for MI, but the trend remained for the highest quintile compared with the lowest when adjusting for traditional risk factors and medical history (HR 0·88; 95 % CI 0·77, 1·00). For women, we found an inverse association between the highest quintile of fatty fish consumption and MI, which remained statistically significant after adjustment for traditional risk factors and medical history (HR 0·78; 95 % CI 0·63, 0·96). Adjustment for dietary variables did not affect the measures of association substantially; however, results for model C were not statistically significant. The test for trends across quintiles was not statistically significant in the adjusted models, and a linear dose–response relationship could not be demonstrated. No consistent associations were seen between consumption of lean fish and MI, for neither men nor women.
Q, quintiles.
* P values test the hypothesis of no trend across quintiles.
† Model A1: crude analysis.
‡ Model A2: adjusted for traditional risk factors including smoking, BMI, waist circumference, physical activity, alcohol intake, educational level and menopausal status (women).
§ Model B: adjusted as model A2 with additional covariates: history of diabetes mellitus, hypertension and hypercholesterolaemia.
|| Model C: adjusted as model A2 with additional dietary covariates: total energy intake, intake of fruits and vegetables and intake of nuts.
In addition, fish intakes were evaluated as continuous variables, modulated as restricted cubic splines with three knots, suggesting an inverse trend between intake of fatty fish and MI for both men and women, whereas lean fish was not associated with MI (Fig. 2).
Dietary intake of marine n-3 PUFA and incident myocardial infarction
We also examined the intakes of individual and total marine n-3 PUFA (EPA, DPA and DHA). The median intake of total marine n-3 PUFA was 0·7 and 0·6 g/d for men and women, respectively. As expected, intake of fatty fish was highly correlated with the calculated intake of marine n-3 PUFA (r 0·93, P<0·001). For men, we observed a trend towards a negative association between EPA, DHA and total marine n-3 PUFA when comparing the highest and lowest quintiles; however, the associations were modest and not statistically significant for any of the models (Table 3). Results were generally more consistent, towards an inverse association, between marine n-3 PUFA and incident MI for women. Accordingly, intake of total and individual marine n-3 PUFA was inversely associated with MI. However, only model B, adjusting for traditional risk factors and medical history, remained statistically significant when comparing the fifth quintile with the first (HR 0·81; 95 % CI 0·66, 0·99). As with intake of fatty fish, the test for trends was not statistically significant across quintiles in the adjusted analyses.
Q, quintiles; DPA, docosapentaenoic acid.
* P values test the hypothesis of no trend across quintiles.
† Model A1: crude analysis.
‡ Model A2: adjusted for traditional risk factors including smoking, BMI, waist circumference, physical activity, alcohol intake, educational level and menopausal status (women).
§ Model B: adjusted as model A2 with additional covariates: history of diabetes mellitus, hypertension and hypercholesterolaemia.
|| Model C: adjusted as model A2 with additional dietary covariates: total energy intake, total intake of SFA, MUFA and PUFA (excl. marine n-3 PUFA) and dietary fibre.
The associations between total marine n-3 PUFA and MI, modulated by restricted cubic splines, are presented in Fig. 2. For women, we found a trend towards an inverse association with MI, whereas for men the association was less strong.
Fatal myocardial infarction
As a secondary analysis, we evaluated the association of fish consumption and intake of marine n-3 PUFA with fatal MI (Table 4). After validation, 580 cases (424 men and 156 women) were categorised as having a fatal MI. Generally, the same tendency towards a negative association for fatty fish intake was observed; however, the CI were broader, and the associations were not statistically significant.
Q, quintiles.
* P values test the hypothesis of no trend across quintiles.
† Model A1: crude analysis.
‡ Model A2: adjusted for smoking, BMI, waist circumference, physical activity, alcohol intake, educational level and menopausal status (women).
§ Model B: adjusted as model A2 with additional covariates: history of diabetes mellitus, hypercholesterolaemia and hypertension.
|| Model C: Adjusted as model A2 with additional covariates. For dietary intake of fish, we adjusted for dietary covariates: total energy intake, intake of fruits and vegetables and intake of nuts. For intake of total n-3 PUFA, we adjusted for specific nutrients: total intake/content of SFA, MUFA and PUFA (excl. marine n-3 PUFA) and dietary fibre. Total marine n-3 PUFA was adjusted for total energy intake.
Discussion
In this Danish prospective cohort study conducted in middle-aged men and women, we examined fish consumption and dietary intake of marine n-3 PUFA in relation to risk of MI. Dietary intake of fatty fish was inversely related to incident MI among men and women when comparing the highest and lowest quintiles, although the association only remained statistically significant for women after multivariate adjustments. For women, the same association was shown for total and individual marine n-3 PUFA with no material differences between EPA, DPA and DHA.
Moreover, two studies have been published previously, based on the Diet Cancer and Health cohort, examining the association of fish intake with adipose tissue marine n-3 PUFA content in participants with Acute Coronary Syndrome (ACS)( Reference Bjerregaard, Joensen and Dethlefsen 6 , Reference Joensen, Overvad and Dethlefsen 7 ). In the present study, the follow-up period was extended and the number of cases was larger providing considerably more strength to explore the associations in both men and women. Thus, Bjerregaard et al.( Reference Bjerregaard, Joensen and Dethlefsen 6 ) found an inverse relationship between intake of fatty fish and ACS in men, suggesting a 32 % lower risk from eating a moderate amount of fatty fish, whereas Joensen et al.( Reference Joensen, Overvad and Dethlefsen 7 ) demonstrated a lower and dose-dependent risk of ACS in men with a high content of marine n-3 PUFA in adipose tissue. Findings in women were inconsistent and non-significant in both studies( Reference Bjerregaard, Joensen and Dethlefsen 6 , Reference Joensen, Overvad and Dethlefsen 7 ). In the present, substantially larger, study, we also demonstrated an inverse relationship in men, but the associations were generally attenuated during the longer follow-up period, and our results concerning fatty fish intake suggested a more modest relative risk of 0·88 when comparing the lowest and the highest quintiles in men. In contrast, our findings in women showed a consistent pattern compared with the earlier studies and suggested a 22 % lower risk from high fish intake comparing the highest quintile with the lowest.
There is generally strong supportive evidence from epidemiological studies( Reference Lemaitre, King and Mozaffarian 5 – Reference Streppel, Ocké and Boshuizen 12 , Reference Amiano, Machón and Dorronsoro 15 ) and secondary intervention trials( Reference Burr, Fehily and Gilbert 17 – Reference Saito, Yokoyama and Origasa 19 ) that intake of fish and marine n-3 PUFA is associated with a lower risk of CHD and sudden cardiac death. Thus, in 2004, He et al. conducted a meta-analysis of prospective cohort studies, suggesting that one fish serving/week is associated with a 15 % lower risk of fatal CHD and 2–4 servings/week with a 23 % lower risk. Today, both the American Heart Association( Reference Kris-Etherton, Harris and Appel 27 ) and the European Society of Cardiology( Reference Catapano, Reiner and De Backer 28 ) recommend a daily intake of marine n-3 PUFA of 1 g/d for secondary prevention of CHD.
Recent clinical trials have questioned the beneficial effects of n-3 PUFA supplements( Reference Kromhout, Giltay and Geleijnse 20 – Reference Galan, Kesse-Guyot and Czernichow 22 ), and several reasons have been proposed to explain these findings. First of all, methodological variations, different populations and different interventions might explain some of the differences. Notably, the recent trials were all conducted in populations with aggressive background therapy with antihypertensive, antiplatelet and lipid-lowering drugs, thereby diminishing the cardio-protective potential of n-3 PUFA. Furthermore, the effect of n-3 PUFA was mainly seen for fatal CHD, whereas most recent trials have focused on non-fatal or composite end points for CHD, and finally the background dietary fish intake was generally higher in recent trials in accordance with rising public awareness of a healthy lifestyle( Reference Wu and Mozaffarian 29 ). In line with this, a recent meta-analysis reported a modest effect of marine n-3 PUFA on cardiovascular end points( Reference Rizos, Ntzani and Bika 3 ).
Several mechanisms have been suggested to explain the cardio-protective properties attributed to marine n-3 PUFA( Reference De Caterina 2 , Reference Saravanan, Davidson and Schmidt 4 , Reference Mozaffarian and Wu 30 ). These mechanisms may explain possible antithrombotic( Reference Saito, Yokoyama and Origasa 19 , Reference Rodriguez, Sharp and Abbott 31 , Reference Eshak, Iso and Yamagishi 32 ) and/or antiarrhythmic( 18 , Reference London, Albert and Anderson 33 , Reference Christensen 34 ) effects of marine n-3 PUFA that may reduce the risk of CHD. In addition, anti-inflammatory properties have been reported, possibly inferring a stabilising effect of marine n-3 PUFA on human atherosclerotic plaques( Reference Thies, Garry and Yaqoob 35 , Reference Calder 36 ) that may decrease the risk of plaque rupture, and thus MI and CHD. Finally, marine n-3 PUFA also lower plasma TAG( Reference Eslick, Howe and Smith 37 ), increase serum adiponectin( Reference Gammelmark, Madsen and Varming 38 , Reference Wu, Cahill and Mozaffarian 39 ) and may slightly reduce blood pressure( Reference De Caterina 2 ). The mechanisms by which n-3 PUFA interact with the risk of MI in the present study are uncertain, but the analyses suggest that the content of marine n-3 PUFA is important, as the inverse relationship between fish intake and MI was observed for fatty fish and not lean fish. Furthermore, intake of fatty fish was highly correlated with intake of total and individual n-3 PUFA (EPA and DHA in particular). A few studies have examined the effect of individual marine n-3 PUFA, as most trials have examined an intervention consisting of a combination of EPA and DHA, as these are the major marine n-3 PUFA found in seafood and fish oil. However, a large intervention trial in a Japanese population used a supplement of purified EPA and produced a significant reduction in major cardiovascular events, suggesting anti-atherosclerotic effects of EPA independently of other marine n-3 PUFA( Reference Saito, Yokoyama and Origasa 19 ). Accordingly, important differential effects have been suggested between the major n-3 PUFA, but more studies on individual n-3 PUFA are warranted( Reference Mozaffarian and Wu 40 ). In the present study, we showed that EPA, DPA and DHA were similarly related to MI, but the study design did not allow for further investigation into the mechanistic aspects of individual n-3 PUFA.
Strengths and limitations
This study was based on a large prospective cohort study and holds the advantages of the prospective design.
The dietary intake of fish and marine n-3 PUFA was evaluated in a detailed manner. First, we assessed fish intake using detailed semi-quantitative FFQ including twenty-six questions concerning fish intake. This allowed us to differentiate by types of fish, thereby grouping fish consumption into fatty and lean fish depending on the content of marine n-3 PUFA. Second, we calculated the intake of major marine n-3 PUFA (EPA, DPA and DHA), to assess these fatty acids individually.
There was a limited loss to follow-up, and the assessment of outcome data was thorough and complete. All outcome data from the National Patient Registry or Causes of Death Registry were either examined from medical records or from a complete list of diagnoses and medical procedure codes, ensuring high validity of cases.
Adjustment for potential confounding was applied in different steps allowing for a more detailed interpretation of the results. In model A2, we adjusted for traditional risk factors for MI, which has a clear and straightforward interpretation. In model B, we applied a second layer of variables adjusting for medical history. These variables are normally considered traditional risk factors for MI and potential confounders, but at the same time may represent intermediate steps in causal pathways by which n-3 PUFA affect the risk of MI. In our opinion, model B represents the most complete analysis including important covariates, and the risk of introducing bias by including intermediate variables is outweighed by the risk of residual confounding by not including these variables. This is, however, open for discussion. Finally, we included dietary variables in addition to the traditional risk factors from model A2 (model C). This model implies adjustment for potential confounding from other aspects of the diet, but it may also introduce dietary patterns that are less comparable with the ordinary dietary pattern. Generally, the differences in measures of association between models were moderate or small, suggesting that confounding was not a major concern in this study.
This study also has certain limitations. Although age was evenly distributed among men and women, there was a markedly higher proportion of male cases and there were relatively few female cases, which made the CI wider for measures of association when analysing data in women, particularly fatal cases. The median follow-up period was 17·0 years, and dietary measures were not assessed during the study period. A long follow-up period allowed us to accumulate more outcome events, but the participants might have changed their diet over time. Furthermore, changes in standard medical care and general changes in lifestyle and public awareness of disease prevention might have influenced the participants’ risk profile. To address this issue, we performed supplementary analysis by stratifying date of birth and testing for interaction from date of birth. No significant interaction was detected, and stratification did not affect the measures of association. Another concern when using FFQ is the chance of measurement error and various sources of bias, and evaluating biomarkers of marine n-3 PUFA intake would add strength to the dietary data. In this article we do not present data on biomarkers of n-3 PUFA, but our group recently published an article investigating the association between adipose tissue content of marine n-3 PUFA and MI, supporting the findings of this dietary study( Reference Gammelmark, Nielsen and Bork 41 ).
Conclusions
In this prospective cohort study, we found a high intake of fatty fish to be inversely related to incident MI in both men and women when comparing the highest and lowest quintiles. However, a clear dose–response relationship could not be established, and the test for trends across quintiles was not statistically significant in the adjusted analyses. Lean fish was not associated with MI. This study supports the current view that consumption of fatty fish may protect against MI.
Acknowledgements
This study was supported by a research grant from The Danish Heart Association, Copenhagen, Denmark, and the Hertha Christensen Foundation, Aalborg, Denmark. The Diet, Cancer and Health study was funded by the Danish Cancer Society. The sponsors neither had influence on the design and conduct of the study nor the writing of the manuscript.
All the authors contributed to the conception and planning of the study. A. G. and S. L.-C. were responsible for the statistical analysis of the data, and all authors were involved in interpretation of the data and writing of the manuscript. A. G. wrote the first draft of the manuscript.
The authors declare that there are no conflicts of interest regarding the present study.
Supplementary Material
For supplementary material/s referred to in this article, please visit http://dx.doi.org/10.1017/S000711451600180X