Pilot study of omega-3 fatty acid supplements in sickle cell disease

Okpala, Iheanyi; Ibegbulam, Obike; Duru, Augustine Nwakuche; Ocheni, S; Emodi, IJ; Ikefuna, AN; Garba, Umar; Asinobi, Isaac Nwabueze; Madu, Anazoeze Jude; Okoye, Augustine Ejike; Nwagha, Theresa Ukamaka; Oguonu, Uche; Uamai, Ify; Agwu, Obineche; Nonyelu, Charles; Anike, Uche; Akaba, Kingsley; Anigbo, Chukwudi; Chukwura, Awele; Ugwu, Ogechukwu; Herrada, S C

doi:10.1111/j.1600-0463.2011.02751.x

Cited by 28 publications

(23 citation statements)

References 21 publications

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“…On the other hand, treatment with n−3 fatty acids resulted in lower but not significant levels of CRP or platelet count compared to untreated patients. This finding is consistent with results reported from studies on healthy adults [35], patients with chronic nonautoimmune disease [36] and SCD patients [37]. It is possible that a larger sample size is needed to elucidate the effect of supplementation on variables of huge inter-individual variations such as platelet count.…”

Section: Discussionsupporting

confidence: 91%

“…Interestingly, SCD patients with PHT have higher levels of markers of endothelial activation, coagulation activation and other inflammatory markers than SCD patients without PHT. Hence the clinical importance of the findings of this study, besides supporting previous reports about the positive therapeutic effect of n − 3 fatty acids in SCD [16,18,19,37], that it suggests high DHA n − 3 supplement as a potential intervention to prevent PHT, stroke and other SCD vasculopathy-related complications.…”

Section: Discussionsupporting

confidence: 88%

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Omega 3 (n−3) fatty acids down-regulate nuclear factor-kappa B (NF-κB) gene and blood cell adhesion molecule expression in patients with homozygous sickle cell disease

Daak

Elderdery

Elbashir

et al. 2015

Blood Cells, Molecules, and Diseases

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Chronic inflammation and reduced blood levels of omega-3 fatty acids (n−3) are known characteristics of sickle cell disease (SCD).The anti-inflammatory properties of n−3 fatty acids are well recognized. Omega-3 treated (n = 24), hydroxyurea (HU) treated (n = 18), and n−3 untreated (n = 21) homozygous SCD patients (HbSS) and healthy (HbAA) controls (n = 25) matched for age (5-16 years), gender and socioeconomic status were studied. According to age (5-10) or (11-16) years, two or three capsules containing 277.8 mg docosahexaenoic (DHA) and 39.0 mg eicosapentaenoic (EPA) or high oleic acid placebo (41%) were assigned to n − 3 treated and n − 3 untreated groups, respectively. Hydroxyurea treated group was on dosage more than 20 mg/kg/day. The effect of supplementation on systemic and blood cell markers of inflammation was investigated. The n− 3 treated group had higher levels of DHA and EPA (p b 0.001) and lower white blood cell count and monocyte integrin (p b 0.05) compared with the n−3 untreated. No difference was detected between the two groups regarding C-reactive protein, granulocytes integrin and selectin, plasma tumour necrosis factor-α and interleukin-10. The n−3 treated group had lowered nuclear factor-kappa B (NF-κB) gene expression compared to n−3 untreated and HU treated groups (p b 0.05). This study provides evidence that supplementation with n− 3 fatty acids may ameliorate inflammation and blood cell adhesion in patients with SCD.

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Section: Discussionsupporting

confidence: 91%

Section: Discussionsupporting

confidence: 88%

Omega 3 (n−3) fatty acids down-regulate nuclear factor-kappa B (NF-κB) gene and blood cell adhesion molecule expression in patients with homozygous sickle cell disease

Daak

Elderdery

Elbashir

et al. 2015

Blood Cells, Molecules, and Diseases

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“…Recent reports on the beneficial effects of ω-3 fatty acid supplementation on the human hematologic phenotype of SCD suggest a possible therapeutic effect of ω-3 fatty acids in SCD. [12][13][14] The present work provides evidence for several relevant mechanisms underlying this potential benefit. We propose that the beneficial role of ω-3 PUFA on SCD vascular dysfunction might be exerted: (i) directly through the reduction of ET-1 expression, which is involved in adaptive inflammation, expression of adhesion molecules such as VCAM-1, and neutrophil chemotaxis; 46 and (ii) indirectly through reduced inflammation and oxidative stress.…”

Section: Discussionmentioning

confidence: 81%

“…10,11 Recently, human studies have demonstrated that supplementation of SCD subjects with fish oil containing ω-3 fatty acids reduces VOC, pain episodes, and blood transfusions. [12][13][14] To date, however, there are insufficient clinical and molecular data to support routine dietary supplementation with fish oil for SCD patients.…”

Section: Introductionmentioning

confidence: 99%

Dietary -3 fatty acids protect against vasculopathy in a transgenic mouse model of sickle cell disease

et al. 2015

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The anemia of sickle cell disease is associated with a severe inflammatory vasculopathy and endothelial dysfunction, which leads to painful and life-threatening clinical complications. Growing evidence supports the anti-inflammatory properties of ω-3 fatty acids in clinical models of endothelial dysfunction. Promising but limited studies show potential therapeutic effects of ω-3 fatty acid supplementation in sickle cell disease. Here, we treated humanized healthy and sickle cell mice for 6 weeks with ω-3 fatty acid diet (fish-oil diet). We found that a ω-3 fatty acid diet: (i) normalizes red cell membrane ω-6/ ω-3 ratio; (ii) reduces neutrophil count; (iii) decreases endothelial activation by targeting endothelin-1 and (iv) improves left ventricular outflow tract dimensions. In a hypoxia-reoxygenation model of acute vaso-occlusive crisis, a ω-3 fatty acid diet reduced systemic and local inflammation and protected against sickle cell-related end-organ injury. Using isolated aortas from sickle cell mice exposed to hypoxia-reoxygenation, we demonstrated a direct impact of a ω-3 fatty acid diet on vascular activation, inflammation, and anti-oxidant systems. Our data provide the rationale for ω-3 dietary supplementation as a therapeutic intervention to reduce vascular dysfunction in sickle cell disease. ABSTRACTmice. 16,17 The animal protocol was approved by the Animal Care and Use Committee of the University of Verona (CIRSAL). Twomonth old animals were fed for 6 weeks with either the standard AIN-93M purified rodent diet (soy-diet with n6/n3 ratio of 8:1 -Dyets Inc., Bethlehem, PA, USA), containing 140 g/kg casein, 1.8 g/kg L-cystine, 100 g/kg sucrose, 465.9 g/kg cornstarch, 155 g/kg dextrose, 40 g/kg soybean oil, 0.8 mg/kg t-butylhydroquinone, 50 g/kg cellulose, 35 g/kg mineral mix, 10 g/kg vitamin mix, and 2.5 g/kg choline bitartrate 18 or the ω-3 FD, an AIN-93M-based purified rodent diet in which all of the calories provided by fat (10%) are replaced by 7.9% from HCO and 2.1% from ω-3 oil (Dyets Inc., Bethlehem, PA, USA). At the end of the 6 weeks of FD supplementation, animals were anesthetized with isofluorane, and whole blood was collected from each mouse via retro-orbital venipuncture by heparinized microcapillaries. Mice were euthanized and organs removed immediately. The organs were divided into two and either frozen immediately in liquid nitrogen or fixed in 10% formalin and embedded in paraffin for histology. Whenever indicated, 6-week old mice were exposed to hypoxia (8% oxygen for 10 h) followed by 3 h of reoxygenation (21% oxygen) (H/R stress) to mimic an acute VOC, as previously described.

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“…In addition, Ren et al [56–58] demonstrated that humans with SCD have decreased omega-3 fatty acids and increased arachidonic acid (an omega-6 fatty acid) in the RBC membrane. To date, trials in humans with SCD have indicated that dietary supplementation with omega-3 fatty acids may reduce severe anemia, vaso-occlusive pain episodes, white blood cell count, and prothrombotic activity [18;52;64]. Of note, these trials did not assess the effect of DHA on RBC structural and functional characteristics.…”

Section: Introductionmentioning

confidence: 99%

Dietary supplementation with docosahexanoic acid (DHA) increases red blood cell membrane flexibility in mice with sickle cell disease

Wandersee

Maciaszek

Giger

et al. 2015

Blood Cells, Molecules, and Diseases

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Humans and mice with sickle cell disease (SCD) have rigid red blood cells (RBCs). Omega-3 fatty acids, such as docosahexanoic acid (DHA), may influence RBC deformability via incorporation into the RBC membrane. In this study, sickle cell (SS) mice were fed natural ingredient rodent diets supplemented with 3% DHA (DHA diet) or a control diet matched in total fat (CTRL diet). After 8 weeks of feeding, we examined the RBCs for: 1) stiffness, as measured by atomic force microscopy; 2) deformability, as measured by ektacytometry; and 3) percent irreversibly sickled RBCs on peripheral blood smears. Using atomic force microscopy, stiffness is increased and deformability decreased in RBCs from SS mice fed CTRL diet compared to wild-type mice. In contrast, RBCs from SS mice fed DHA diet had markedly decreased stiffness and increased deformability compared to RBCs from SS mice fed CTRL diet. Furthermore, examination of peripheral blood smears revealed less irreversibly sickled RBCs in SS mice fed DHA diet as compared to CTRL diet. In summary, our findings indicate that DHA supplementation improves RBC flexibility and reduces irreversibly sickled cells by 40% in SS mice. These results point to potential therapeutic benefits of dietary omega-3 fatty acids in SCD.

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Pilot study of omega-3 fatty acid supplements in sickle cell disease

Cited by 28 publications

References 21 publications

Omega 3 (n−3) fatty acids down-regulate nuclear factor-kappa B (NF-κB) gene and blood cell adhesion molecule expression in patients with homozygous sickle cell disease

Omega 3 (n−3) fatty acids down-regulate nuclear factor-kappa B (NF-κB) gene and blood cell adhesion molecule expression in patients with homozygous sickle cell disease

Dietary -3 fatty acids protect against vasculopathy in a transgenic mouse model of sickle cell disease

Dietary supplementation with docosahexanoic acid (DHA) increases red blood cell membrane flexibility in mice with sickle cell disease

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