Impact of a (poly)phenol-rich extract from the brown algae Ascophyllum nodosum on DNA damage and antioxidant activity in an overweight or obese population: a randomized controlled trial

Author:

Baldrick Francina R1,McFadden Kevin1,Ibars Maria1,Sung Chris1,Moffatt Tanya1,Megarry Kate1,Thomas Keith2,Mitchell Peter1,Wallace Julie M W1,Pourshahidi L Kirsty1,Ternan Nigel G1,Corona Giulia34,Spencer Jeremy3,Yaqoob Parveen3,Hotchkiss Sarah5,Campbell Ross5,Moreno-Rojas José Manuel6,Cuevas Francisco Julián6,Pereira-Caro Gema6,Rowland Ian3,Gill Chris I R1

Affiliation:

1. Nutrition Innovation Centre for Food and Health, University of Ulster, Coleraine, United Kingdom

2. School of Biomedical Sciences, Centre for Molecular Biosciences, University of Ulster, Coleraine, United Kingdom

3. Hugh Sinclair Unit of Human Nutrition, Department of Food and Nutritional Sciences, University of Reading, Reading, United Kingdom

4. Health Sciences Research Centre, University of Roehampton, London, United Kingdom

5. CyberColloids Ltd., Carrigaline Industrial Estate, Carrigaline, Ireland

6. Department of Food Science and Health, IFAPA-Alameda del Obispo, Córdoba, Spain

Abstract

AbstractBackgroundEpidemiologic evidence suggests that a diet rich in (poly)phenols has beneficial effects on many chronic diseases. Brown seaweed is a rich source of (poly)phenols.ObjectiveThe aim of this study was to investigate the bioavailability and effect of a brown seaweed (Ascophyllum nodosum) (poly)phenol extract on DNA damage, oxidative stress, and inflammation in vivo.DesignA randomized, double-blind, placebo-controlled crossover trial was conducted in 80 participants aged 30–65 y with a body mass index (in kg/m2) ≥25. The participants consumed either a 400-mg capsule containing 100 mg seaweed (poly)phenol and 300 mg maltodextrin or a 400-mg maltodextrin placebo control capsule daily for an 8-wk period. Bioactivity was assessed with a panel of blood-based markers including lymphocyte DNA damage, plasma oxidant capacity, C-reactive protein (CRP), and inflammatory cytokines. To explore the bioavailability of seaweed phenolics, an untargeted metabolomics analysis of urine and plasma samples after seaweed consumption was determined by ultra-high-performance liquid chromatography–high-resolution mass spectrometry.ResultsConsumption of the seaweed (poly)phenols resulted in a modest decrease in DNA damage but only in a subset of the total population who were obese. There were no significant changes in CRP, antioxidant status, or inflammatory cytokines. We identified phlorotannin metabolites that are considered potential biomarkers of seaweed consumption including pyrogallol/phloroglucinol-sulfate, hydroxytrifurahol A-glucuronide, dioxinodehydroeckol-glucuronide, diphlorethol sulfates, C-O-C dimer of phloroglucinol sulfate, and C-O-C dimer of phloroglucinol.ConclusionsTo the best of our knowledge, this work represents the first comprehensive study investigating the bioactivity and bioavailability of seaweed (poly)phenolics in human participants. We identified several potential biomarkers of seaweed consumption. Intriguingly, the modest improvements in DNA damage were observed only in the obese subset of the total population. The subgroup analysis should be considered exploratory because it was not preplanned; therefore, it was not powered adequately. Elucidation of the biology underpinning this observation will require participant stratification according to weight in future studies. This trial was registered at clinicaltrials.gov as NCT02295878.

Funder

European Union Seventh Framework Program

Spanish Ministry of Economy and Competitiveness

Publisher

Oxford University Press (OUP)

Subject

Nutrition and Dietetics,Medicine (miscellaneous)

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