| Literature DB >> 35276928 |
Giuseppe Banderali1, Maria Elena Capra2,3, Claudia Viggiano1, Giacomo Biasucci2, Cristina Pederiva1.
Abstract
Coronary heart disease (CHD) is the main cause of death and morbidity in the world. Childhood is a critical period during which atherosclerosis may begin to develop; in the presence of familial hypercholesterolaemia (FH), the lifelong elevation of LDL cholesterol levels greatly accelerates atherosclerosis. Lowering LDL-C levels is associated with a well-documented reduction in cardiovascular disease risk. Current guidelines support the dietary and lifestyle approach as the primary strategy of intervention in children and adolescents with FH. Nutraceuticals (functional foods or dietary supplements of plant or microbial origin) are included in the EU guidelines as lifestyle interventions and may provide an additional contribution in reducing LDL levels when pharmacological therapy is not yet indicated. Meta-analyses of randomised clinical trials have demonstrated that the same nutraceuticals improve lipid profile, including lowering LDL-C, total cholesterol and triglyceride levels. In this narrative review, starting from current scientific evidence, we analyse the benefits and limitations of the nutraceuticals in children and adolescents with dyslipidaemia, and we try to evaluate their use and safety in clinical practice.Entities:
Keywords: diet; dyslipidaemia; familial hypercholesterolaemia; nutraceuticals; paediatric
Mesh:
Year: 2022 PMID: 35276928 PMCID: PMC8840379 DOI: 10.3390/nu14030569
Source DB: PubMed Journal: Nutrients ISSN: 2072-6643 Impact factor: 5.717
Nutritional and lifestyle intervention in paediatric patients with hypercholesterolaemia; adapted from Giovannini et al. [5] and Catapano et al. [6].
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Nutritional treatment is the milestone intervention in paediatric patients at increased CVD risk. Dietary-nutritional intervention in children with dyslipidaemia has the main objective to establish correct eating habits that are most likely to be maintained over time until adulthood. It is recommended to limit the consumption of foods with high content of saturated fats, as they are the main responsible for the increase in cholesterolaemia. A prudent low-fat diet is recommended, encouraging the intake of fruits, vegetables, unrefined grains, pulses, fish and meats. The traditional Mediterranean diet represents the ideal model because it proposes a diet rich in these foods, reduced consumption of salt and condiments in the preparation of foods, a preference for extra virgin olive oil and steamed, baked and stewed foods. Physical activity should be promoted, and conditions related to the CVD risk should be limited, such as sedentary life, cigarette smoke (also passive), obesity, hypertension and diabetes. |
Figure 1Use of nutraceuticals in dyslipidaemia in childhood.
Nutraceuticals effect on lipid profile.
| Reduce Total Cholesterol | Reduce LDL Cholesterol | Reduce Triglycerides | Increase HDL Cholesterol | |
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+ means positive effect.
Figure 2Nutraceuticals’ inhibitors of intestinal absorption.
Figure 3Nutraceuticals’ inhibitors of liver cholesterol synthesis.
Figure 4Nutraceuticals’ inducer of LDL-cholesterol excretion.
Figure 5Nutraceuticals with mixed action.
Characteristics of studies about the effect of nutraceuticals in paediatric subjects with dyslipidaemia.
| Nutraceuticals | Type of Study | Aim | Casuistry | Dose and Duration of the Intervention | Effects | Reference |
|---|---|---|---|---|---|---|
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| DB-CO- | Lipid-lowering effect of cereals added to psyllium | 32 children | 8-week diet: 58 g of cereals added to psyllium (6.4 g) or to placebo | ↓ TC: −5% | Davidson MH et al., Am J Clin Nutr |
| RCT | Reduction of CT and LDL-C after integration with psyllium | 36 children | Age ≤ 7 years: 5 g/die | ↓ TC: −18% | Glassman M | |
| SB-RCT | Effectiveness of psyllium in CT and LDL-C reduction | 50 children | CHILD I: all groups. Intervention: cereals containing 3.2 g of psyllium. Duration: 12 weeks | ↓ TC: −9.6% | Williams CL | |
| DB-RCT | Effectiveness of psyllium on LDL-C in Brazilians children and teenagers with dyslipidaemia | 51 children | CHILD II: 6 weeks. Intervention group: 7 g/die of psyllium Control group: 7.0 g/die of cellulose | ↓ TC: −7.7% | Ribas SA | |
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| DB-CO- | Efficacy and tolerability of | 36 FH children | CHILD I diet | ↓ TC: 5.1% | Guardamagna O et al., Nutrition 2013 [ |
| DB-RCT | Lipid-lowering effects of | 132 children | Randomised assignment | GM + CP: | Martino F | |
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| DB-CO-RCT | Lipid-lowering | 30 children | Intervention group: | Intervention group: | Ribas SA |
| DB-CO-RCT | Lipid-lowering | 38 children | CHILD I + | ↓ LDL-C 10.2% | Amundsen AL | |
| CT | Effects of sterols | 64 children | CHILD II | Intervention group: | Garoufi A et al., | |
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| DB-CO-RCT | Efficacy and safety of a combination of red yeast rice extract and policosanols | 80 children | CHILD I | ↓ TC: 18.5% | Guardamagna O et al., NMCD 2011 [ |
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| RCT | The effect of integration | 23 children | Step 1: diet | Step 1: | Weghuber D |
| RCT | The effect of soy on LDL-C levels | 17 children | Soy group: soy-enriched fat modified diet Control group: fat modified diet | LDL-C decrease: statistically significantly greater in the soy group | Helk O et al., Clin Nutr 2020 [ | |
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| DB-CO-RCT | The efficacy of fish oil in lowering TG and impacting lipoprotein particles | 42 children | Intervention group: 4 g daily of fish oil | TG decrease: greater in the intervention group | Gidding SS et al., J Pediatr 2014 [ |
| RCT | The effectiveness of hempseed oil in the modulation of hyperlipidaemia and evaluation of fatty acid composition of red blood cells | 36 children | Control group: CHILD I | Intervention group: | del Bo’ C et al., |
DB—double blind; SB—single blind; CO—cross-over; RCT—randomised controlled trial; CT—controlled trial; ↓—decrease; ↑—increase; FH—familial hypercholesterolaemia; TC—total cholesterol; LDL-C—low-density lipoprotein cholesterol; HDL-C—high-density lipoprotein cholesterol; TG—triglycerides; GM—glucomannan; CP—chromium-polynicotinate; RC—blood red cells; SFA—saturated fatty acids; MUFA—monounsaturated fatty acids; PUFA—polyunsaturated fatty acids.