Meta-analysis studies with normotensive and hypertensive subjects

Different meta-analysis have shown that relatively high doses of omega-3 PUFA, generally more than 3 g/d, can lead to clinically relevant BP reductions in individuals with untreated hypertension. In the meta-analysis of Appel et al., including 17 clinical trials (11 in normotensives and 6 in untreated hypertensive subjects), the reduction in systolic blood pressure (SBP) and diastolic blood pressure (DBP) in hypertensive subjects were 5·5 and 3·5 mmHg, respectively⁽Reference Appel, Miller, Seidler and Whelton¹⁶⁾. Another meta-analysis including 36 studies, 22 of which were double-blind designed and with a duration over 2 weeks, showed a significant 2·1 mmHg reduction in SPB and 1·6 mmHg DBP (1·7/1·5 mmHg in the double-blind studies) with a median consumption of 3·7 g/day of fish oil. The effect was higher in subjects >45 years and in hypertensive volunteers (BP ≥  140/90 mmHg)⁽Reference Geleijnse, Giltay, Grobbee, Donders and Kok¹⁷⁾.

Meta-analysis studies including type 2 diabetic subjects

A meta-analysis of 12 randomized trials performed in patients with type 2 diabetes showed a discrete effect on DBP in five trials ( − 1·79 mmHg, P = 0·05), but not in SBP and heart rate. Mean ω-3 dose was 4·6 g/day, ranging from 3 to 8 g/day. The main limitations of the results were the small number of trials available and the sample size of the studies (mean 30·6, range 23–40)⁽Reference Hartweg, Farmer, Holman and Neil¹⁸⁾.

In a recent meta-analysis including 24 trials, the possible beneficial effect of ω-3 PUFA in patients with type 2 diabetes mellitus was also analyzed⁽Reference Hartweg, Farmera, Holmanb and Neil¹⁹⁾. Only 8 of the 24 trials reported blood pressure changes and a total of 747 participants were studied in the trials. The main results showed that ω-3 supplements did not produce significant changes in SBP or DBP (SBP: − 0·78 mmHg P = 0·44, DBP: − 0·79 P = 0·18). The absence of a dose-dependent analysis is a limitation to the results on blood pressure of this meta-analysis.

Effect of ω-3 supplementation on blood pressure in healthy subjects

In a randomized, placebo-controlled study, 162 halthy subjects received a diet with high proportion of saturated fatty acids or high proportion of monounsaturated fatty acids. Both groups were further randomly assigned to receive supplementation with fish oil (3·6 g n-3 fatty acids/d) or placebo. The main objective was to evaluate the effects of different types of dietary fat on BP in healthy subjects. The results showed that supplementation did not affect blood pressure in healthy volunteers, independent of the amount of fat on diet⁽Reference Rasmussen, Vessby, Uusitupa, Berglund, Pedersen, Riccardi, Rivellese, Tapsell and Hermanen²⁰⁾. Similar results were observed in a smaller and short-term study performed in 37 healthy volunteers using lower dose of ω-3 PUFA (1 g/day)⁽Reference Shah, Ichiuji, Han, Traina, El-Bialy, Meymandi and Wachsner²¹⁾.

Dietary intervention studies in obese subjects with or without hyperlipemia (cross-sectionals and randomized studies)

In a small dietary intervention study⁽Reference Bao, Mori, Burke, Puddey and Beilin²²⁾, 69 volunteers with overweight and treated hypertension, were randomized to 4 different diets: 1) fish diet containing 3·65 g/day of ω-3 PUFA; 2) low-calories diet; 3) combination of both diets and 4) control diet. Subjects consuming high amount of ω-3 reduced SBP and DBP by 6·0 and 3·0 mmHg respectively, similar to the reduction observed in the low-calories diet (5·5/2·2 mmHg); however, the reduction was higher with the combination of both diets (13·0/9·3 mmHg). Heart rate significantly decreased in the fish diet group (3·1 bpm sd 1·4). In conclusion, the combination of fish and low-calories diet was additive in terms of effects on blood pressure, so these results may be relevant in the management of patients with metabolic syndrome.

Ramel A et al. ⁽Reference Ramel, Pumberger, Martinez, Kiely, Bandarra and Thorsdottir²³⁾ analyzed the association in a cross-sectional study between diet, ω-3 PUFA index in red blood cell membranes and cardiovascular risk factors in 324 subjects aged 30–35 years and overweight in Spain, Iceland and Ireland. None of the participants had type 2 diabetes and 32 % had high blood pressure. There were no association between red blood cell ω-3 fatty acid composition (ω-3 index) and systolic or diastolic blood pressure. Body mass index was significantly associated with increased blood pressure but no with cholesterol measures.

Recently, it has been published the LIPGENE dietary intervention study⁽Reference Gulseth, Gjelstad, Tierney, Shaw, Helal, Hees, Delgado, Leszczynska-Golabek, Karlström, Lovegrove, Defoort, Blaak, Lopez-Miranda, Dembinska-Kiec, Risérus, Roche, Birkeland and Br Drevon²⁴⁾. This study evaluated the effect of ω-3 PUFA on blood pressure in individuals with metabolic syndrome for 12 weeks, randomizing volunteers to one of four isoenergetic diets avoiding weight loss bias. In two diets, 38 % of total energy came from fat: one high in saturated fatty acids and another high in monounsaturated fatty acids. In the other 2 diets 20 % of energy came from fat: one supplemented with 1–2 g/day of ω-3 and one supplemented with oleic acid or sunflower oil. There were no differences in systolic and diastolic blood pressure between the different diets, and the authors' suggested that the dose of ω-3 was too low compared with other studies, or perhaps the absence of weight loss was important taking into account the relationship between weight loss and blood pressure reduction.

The effect of ω-3 in blood pressure in subjects with hyperlipidemia has been controversial. In a retrospective study, the effect of ω-3 PUFA supplementation during 12 months on blood pressure was evaluated in 111 subjects with hypertriglyceridemia and high-normal blood pressure without treatment. Subjects received 2 g/day of ω-3 PUFA, containing at least 85 % EPA and DHA with a ratio of 0·9:1·5. The results showed a slight but significant reduction of systolic and diastolic blood pressure (2·7 ± 2·5, 1·4 ± 4·2, respectively). In men, there were a significant association between baseline triglyceride levels with change in systolic blood pressure, which might be of interest in the selection of specific subjects in which ω-3 supplementation could be of maximum benefit⁽Reference Cicero, Derosa, Di Gregorio, Bove, Gaddi and Borghi²⁵⁾.

In another study, 60 hyperlipidemic patients were randomly assigned to one of 4 groups: placebo, fish oil (1·4 g/day of ω-3), plant sterols (2 g/day) and the combination of fish oil and plant sterols. There was a non significant trend to decrease SBP and DBP in the groups containing ω-3 PUFA⁽Reference Micallef and Garg²⁶⁾. On the other hand, it has been shown that long-term administration of low dose of ω-3 PUFA (1 g/day) do not reduce blood pressure in overweight volunteers with hypertriglyceridemia followed-up during 6 months⁽Reference Murphy, Meyer, Mori, Burke, Mansour, Patch, Tapsell, Noakes, Clifton, Barden, Puddey, Beilin and Howe²⁷⁾.

Differential effects of EPA and DHA on blood pressure

Some clinical trials have suggested that EPA and DHA have differential hemodynamic effects. DHA may be more favorable in reducing blood pressure and heart rate, although not all trials show conclusive results. In this sense, Theobald H et al., conducted a randomized, double-blind and placebo-controlled study in which 38 healthy subjects were treated for 3 months with 0·7 g/day of DHA vs. placebo⁽Reference Theobald Middleaged, Goodall, Sattar, Talbot, Chowienczyk and Sanders²⁸⁾. Diastolic blood pressure in patients treated with DHA fell 3·3 mmHg, in comparison with placebo (P < 0·01). There were no significant differences in resting heart rate and SBP. Another study using algae oil (1·5 gr/day of DHA and 0·6 g/day of docosapentaenoic acid) showed no differences in blood pressure between the control group and the group supplemented with the oil, perhaps due to low doses of ω-3 provided either by the combination with ω-6⁽Reference Sanders, Gleason, Griffin and Miller²⁹⁾.

The effect of ω-3 on blood pressure has also been analysed in 59 overweight men with hyperlipidemia randomized to receive either 4 g/day of EPA, 4 g/day of DHA or olive oil (as control group) during 6 weeks, maintaining the rest of nutrients in their regular diets. The study showed that only in the DHA group there was a significant reduction of blood pressure and heart rate compared with placebo. The average reduction in SBP/DBP was 5·8/3·3 mmHg, while heart rate fell 3·5 (sd 0·8 bpm). EPA did not show statistically significant effect on either blood pressure or on heart rate.⁽Reference Mori, Bao, Burke, Puddey and Beilin³⁰⁾

Effect of ω-3 in blood pressure in other populations

Recently, Vernaglione L. et al. ⁽Reference Vernaglione, Cristofano and Chimienti³¹⁾ published a prospective study on the effects on blood pressure and other variables in 24 patients on hemodialysis who were supplemented with ω-3. The study was designed sequentially, so after baseline evaluation patients had to follow consecutive periods of 4 months with different supplements: 2 g/day of olive oil followed by 2 g/day of ω-3 supplements and finally back to 2 g/day of olive oil. Both SBP and DBP were significantly lower (P < 0·05) at the end of the supplementation period with ω-3. Systolic blood pressure diminished from 131 ± 17·8 mmHg in the first phase to 122 mmHg (sd 12·8) in the second phase and rose to 129 ± 13·2 mmHg. The effect on DBP was in the same direction: 83 ± 16·3 mmHg in the first phase, 71 ± 14·8 mmHg in the second phase and 79 ± 6·5 mmHg in the last period of the study.