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6. Effects of Dietary Fibers on Short-Chain Fatty Acids and Gut Microbiota Composition in Healthy Adults: A Systematic Review

Author

Vinelli V., Biscotti P., Martini D., Del Bo' C., Marino M., Merono T., Nikoloudaki O., Calabrese F. M., Turroni S., Taverniti V., Caballero A. U., Andres-Lacueva C., Porrini M., Gobbetti M., De Angelis M., Brigidi P., Pinart M., Nimptsch K., Guglielmetti S., Riso P., Vinelli V., Biscotti P., Martini D., Del Bo' C., Marino M., Merono T., Nikoloudaki O., Calabrese F.M., Turroni S., Taverniti V., Caballero A.U., Andres-Lacueva C., Porrini M., Gobbetti M., De Angelis M., Brigidi P., Pinart M., Nimptsch K., Guglielmetti S., and Riso P.

Subjects
Adult, Dietary Fiber, Prebiotics, human gut microbiota, intervention studie, Microbiota, prebiotic, short chain fatty acid, Humans, Fatty Acids, Volatile, Human, Gastrointestinal Microbiome
Abstract

There is an increasing interest in investigating dietary strategies able to modulate the gut microbial ecosystem which, in turn, may play a key role in human health. Dietary fibers (DFs) are widely recognized as molecules with prebiotic effects. The main objective of this systematic review was to: (i) analyze the results available on the impact of DF intervention on short chain fatty acids (SCFAs) production; (ii) evaluate the interplay between the type of DF intervention, the gut microbiota composition and its metabolic activities, and any other health associated outcome evaluated in the host. To this aim, initially, a comprehensive database of literature on human intervention studies assessing the effect of confirmed and candidate prebiotics on the microbial ecosystem was developed. Subsequently, studies performed on DFs and analyzing at least the impact on SCFA levels were extracted from the database. A total of 44 studies from 42 manuscripts were selected for the analysis. Among the different types of fiber, inulin was the DF investigated the most (n = 11). Regarding the results obtained on the ability of fiber to modulate total SCFAs, seven studies reported a significant increase, while no significant changes were reported in five studies, depending on the analytical methodology used. A total of 26 studies did not show significant differences in individual SCFAs, while the others reported significant differences for one or more SCFAs. The effect of DF interventions on the SCFA profile seemed to be strictly dependent on the dose and the type and structure of DFs. Overall, these results underline that, although affecting microbiota composition and derived metabolites, DFs do not produce univocal significant increase in SCFA levels in apparently healthy adults. In this regard, several factors (i.e., related to the study protocols and analytical methods) have been identified that could have affected the results obtained in the studies evaluated. Future studies are needed to better elucidate the relationship between DFs and gut microbiota in terms of SCFA production and impact on health-related markers.

Published
2022

9. Estimated intakes of nutrients and polyphenols in participants completing the maple randomised controlled trial and its relevance for the future development of dietary guidelines for the older subjects

Author

Martini, D, Bernardi, S, Del Bo', C, Liberona, N, Zamora-Ros, R, Tucci, M, Cherubini, A, Porrini, M, Gargari, G, Gonzalez-Dominguez, R, Peron, G, Kirkup, B, Kroon, P, Andres-Lacueva, C, Guglielmetti, S, Riso, P, Martini D., Bernardi S., Del Bo' C., Liberona N. H., Zamora-Ros R., Tucci M., Cherubini A., Porrini M., Gargari G., Gonzalez-Dominguez R., Peron G., Kirkup B., Kroon P. A., Andres-Lacueva C., Guglielmetti S., Riso P., Martini, D, Bernardi, S, Del Bo', C, Liberona, N, Zamora-Ros, R, Tucci, M, Cherubini, A, Porrini, M, Gargari, G, Gonzalez-Dominguez, R, Peron, G, Kirkup, B, Kroon, P, Andres-Lacueva, C, Guglielmetti, S, Riso, P, Martini D., Bernardi S., Del Bo' C., Liberona N. H., Zamora-Ros R., Tucci M., Cherubini A., Porrini M., Gargari G., Gonzalez-Dominguez R., Peron G., Kirkup B., Kroon P. A., Andres-Lacueva C., Guglielmetti S., and Riso P.

Abstract

The evaluation of food intake in older subjects is crucial in order to be able to verify adherence to nutritional recommendations. In this context, estimation of the intake of specific dietary bioactives, such as polyphenols, although particularly challenging, is necessary to plan possible intervention strategies to increase their intake. The aims of the present study were to: (i) evaluate the nutritional composition of dietary menus provided in a residential care setting; (ii) estimate the actual intake of nutrients and polyphenols in a group of older subjects participating in the MaPLE study; and (iii) investigate the impact of an eight-week polyphenol-rich dietary pattern, compared to an eight-week control diet, on overall nutrient and polyphenol intake in older participants. The menus served to the participants provided ~770 mg per day of total polyphenols on average with small variations between seasons. The analysis of real consumption, measured using weighed food diaries, demonstrated a lower nutrient (~20%) and polyphenol intake (~15%) compared to that provided by the menus. The feasibility of dietary patterns that enable an increase in polyphenol intake with putative health benefits for age-related conditions is discussed, with a perspective to developing dietary guidelines for this target population.

Published
2020

10. Increased Intestinal Permeability in Older Subjects Impacts the Beneficial Effects of Dietary Polyphenols by Modulating Their Bioavailability

Author

Hidalgo-Liberona, N, Gonzalez-Dominguez, R, Vegas, E, Riso, P, Del Bo', C, Bernardi, S, Peron, G, Guglielmetti, S, Gargari, G, Kroon, P, Cherubini, A, Andres-Lacueva, C, Hidalgo-Liberona N., Gonzalez-Dominguez R., Vegas E., Riso P., Del Bo' C., Bernardi S., Peron G., Guglielmetti S., Gargari G., Kroon P. A., Cherubini A., Andres-Lacueva C., Hidalgo-Liberona, N, Gonzalez-Dominguez, R, Vegas, E, Riso, P, Del Bo', C, Bernardi, S, Peron, G, Guglielmetti, S, Gargari, G, Kroon, P, Cherubini, A, Andres-Lacueva, C, Hidalgo-Liberona N., Gonzalez-Dominguez R., Vegas E., Riso P., Del Bo' C., Bernardi S., Peron G., Guglielmetti S., Gargari G., Kroon P. A., Cherubini A., and Andres-Lacueva C.

Abstract

Polyphenols have great potential in regulating intestinal health and ameliorating pathological conditions related to increased intestinal permeability (IP). However, the efficacy of dietary interventions with these phytochemicals may significantly be influenced by interindividual variability factors affecting their bioavailability and consequent biological activity. In the present study, urine samples collected from older subjects undergoing a crossover intervention trial with polyphenol-rich foods were subjected to metabolomics analysis for investigating the impact of increased IP on the bioavailability of polyphenols. Interestingly, urinary levels of phase II and microbiota-derived metabolites were significantly different between subjects with healthier intestinal barrier integrity and those with increased IP disruption. Our results support that this IP-dependent impaired bioavailability of polyphenols could be attributed to disturbances in the gut microbial metabolism and phase II methylation processes. Furthermore, we also observed that microbiota-derived metabolites could be largely responsible for the biological activity elicited by dietary polyphenols against age-related disrupted IP.

Published
2020

11. Métabolites dérivés du microbiote intestinal et déclin cognitif : une exploration de l’axe intestin-cerveau

Author

Neuffer, J., primary, Gonzalez-Dominguez, R., additional, Lefèvre-Arbogast, S., additional, Low, D.Y., additional, Driollet, B., additional, Helmer, C., additional, Du Preez, A., additional, De Lucia, C., additional, Ruigrok, S., additional, Altendorfer, B., additional, Aigner, L., additional, Lucassen, P.J., additional, Korosi, A., additional, Thuret, S., additional, Manach, C., additional, Pallas, M., additional, Urpi-Sarda, M., additional, Sanchez-Pla, A., additional, Andres-Lacueva, C., additional, and Samieri, C., additional

Published
2022
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14. Association between Food Intake, Clinical and Metabolic Markers and DNA Damage in Older Subjects

Author

Del Bo', C., Martini, D., Bernardi, S., Gigliotti, L., Marino, M., Gargari, G., Merono, T., Hidalgo-Liberona, N., Andres-Lacueva, C., Kroon, P. A., Cherubini, A., Guglielmetti, S., Porrini, M., and Riso, P.

Subjects
Aging, aging, Polyphenols, RM1-950, Persones grans, Article, Envelliment, Polifenols, metabolic markers, DNA damage, older subjects, Therapeutics. Pharmacology, Older people, diet
Abstract

The use of DNA damage as marker of oxidative stress, metabolic dysfunction and age-related diseases is debated. The present study aimed at assessing the level of DNA damage (evaluated as DNA strand-breaks, endogenous and oxidatively-induced DNA damage) in a group of older subjects with intestinal permeability enrolled within the MaPLE (Gut and Blood Microbiomics for Studying the Effect of a Polyphenol-Rich Dietary Pattern on Intestinal Permeability in the Elderly) intervention trial, to evaluate its association with clinical, metabolic and dietary markers. DNA damage in peripheral blood mononuclear cells was assessed by the comet assay in 49 older subjects participating in the study. Clinical and metabolic markers, markers of inflammation, vascular function and intestinal permeability were determined in serum. Food intake was estimated by weighted food diaries. On the whole, a trend towards higher levels of DNA damage was observed in men compared to women (p = 0.071). A positive association between DNA damage and clinical/metabolic markers (e.g., uric acid, lipid profile) and an inverse association with dietary markers (e.g., vitamin C, E, B6, folates) were found and differed based on sex. By considering the importance of DNA stability during aging, the results obtained on sex differences and the potential role of dietary and metabolic factors on DNA damage underline the need for further investigations in a larger group of older adults to confirm the associations found and to promote preventive strategies.

Published
2021

16. Bacterial DNAemia is associated with serum zonulin levels in older subjects

Author

Gargari, G, Mantegazza, G, Taverniti, V, Del Bó, C, Bernardi, S, Andres-Lacueva, C, González-Domínguez, R, Kroon, P, Winterbone, M, Cherubini, A, Riso, P, Guglielmetti, S, Kroon, PA, Winterbone, MS, Gargari, G, Mantegazza, G, Taverniti, V, Del Bó, C, Bernardi, S, Andres-Lacueva, C, González-Domínguez, R, Kroon, P, Winterbone, M, Cherubini, A, Riso, P, Guglielmetti, S, Kroon, PA, and Winterbone, MS

Abstract

The increased presence of bacteria in blood is a plausible contributing factor in the development and progression of aging-associated diseases. In this context, we performed the quantification and the taxonomic profiling of the bacterial DNA in blood samples collected from forty-three older subjects enrolled in a nursing home. Quantitative PCR targeting the 16S rRNA gene revealed that all samples contained detectable amounts of bacterial DNA with a concentration that varied considerably between subjects. Correlation analyses revealed that the bacterial DNAemia (expressed as concentration of 16S rRNA gene copies in blood) significantly associated with the serum levels of zonulin, a marker of intestinal permeability. This result was confirmed by the analysis of a second set of blood samples collected from the same subjects. 16S rRNA gene profiling revealed that most of the bacterial DNA detected in blood was ascribable to the phylum Proteobacteria with a predominance of the genus Pseudomonas. Several control samples were also analyzed to assess the influence of contaminant bacterial DNA potentially originating from reagents and materials. The data reported here suggest that para-cellular permeability of epithelial (and, potentially, endothelial) cell layers may play an important role in bacterial migration into the bloodstream. Bacterial DNAemia is likely to impact on several aspects of host physiology and could underpin the development and prognosis of various diseases in older subjects.

Published
2021

17. A polyphenol-rich dietary pattern improves intestinal permeability, evaluated as serum zonulin levels, in older subjects : the MaPLE randomised controlled trial

Author

Del Bo', C, Bernardi, S, Cherubini, A, Porrini, M, Gargari, G, Hidalgo-Liberona, N, Gonzalez-Dominguez, R, Zamora-Ros, R, Peron, G, Marino, M, Gigliotti, L, Winterbone, M, Kirkup, B, Kroon, P, Andres-Lacueva, C, Guglielmetti, S, Riso, P, Cristian Del Bo', Stefano Bernardi, Antonio Cherubini, Marisa Porrini, Giorgio Gargari, Nicole Hidalgo-Liberona, Raul Gonzalez-Dominguez, Raul Zamora-Ros, Gregorio Peron, Mirko Marino, Letizia Gigliotti, Mark S. Winterbone, Benjamin Kirkup, Paul A. Kroon, Cristina Andres-Lacueva, Simone Guglielmetti, Patrizia Riso, Del Bo', C, Bernardi, S, Cherubini, A, Porrini, M, Gargari, G, Hidalgo-Liberona, N, Gonzalez-Dominguez, R, Zamora-Ros, R, Peron, G, Marino, M, Gigliotti, L, Winterbone, M, Kirkup, B, Kroon, P, Andres-Lacueva, C, Guglielmetti, S, Riso, P, Cristian Del Bo', Stefano Bernardi, Antonio Cherubini, Marisa Porrini, Giorgio Gargari, Nicole Hidalgo-Liberona, Raul Gonzalez-Dominguez, Raul Zamora-Ros, Gregorio Peron, Mirko Marino, Letizia Gigliotti, Mark S. Winterbone, Benjamin Kirkup, Paul A. Kroon, Cristina Andres-Lacueva, Simone Guglielmetti, and Patrizia Riso

Abstract

Background & aim: Increased intestinal permeability (IP) can occur in older people and contribute to the activation of the immune system and inflammation. Dietary interventions may represent a potential strategy to reduce IP. In this regard, specific food bioactives such as polyphenols have been proposed as potential IP modulator due to their ability to affect several critical targets and pathways that control IP. The trial aimed to test the hypothesis that a polyphenol-rich dietary pattern can decrease serum zonulin levels, an IP surrogate marker involved in tight junction modulation, and can beneficially alter the intestinal microbiota, and IP-associated biochemical and clinical markers in older subjects. Methods: A randomised, controlled, cross-over intervention trial was performed. Sixty-six subjects (aged ≥ 60 y) with increased IP based on serum zonulin levels, were randomly allocated to one of the two arms of the intervention consisting of a control diet (C-diet) vs. a polyphenol-rich diet (PR-diet). Each intervention was 8-week long and separated by an 8-week wash out period. At the beginning and at the end of each intervention period, serum samples were collected for the quantification of zonulin and other biological markers. Faecal samples were also collected to investigate the intestinal microbial ecosystem. In addition, anthropometrical/physical/biochemical parameters and food intake were evaluated. Results: Fifty-one subjects successfully completed the intervention and a high compliance to the dietary protocols was demonstrated. Overall, polyphenol intake significantly increased from a mean of 812 mg/day in the C diet to 1391 mg/day in the PR-diet. Two-way analysis of variance showed a significant effect of treatment (p = 0.008) and treatment × time interaction (p = 0.025) on serum zonulin levels, which decreased after the 8-week PR-diet. In addition, a treatment × time interaction was observed showing a reduction of diastolic blood pressure (p = 0.0

Published
2021

18. Association between food intake, clinical and metabolic markers and DNA damage in older subjects

Author

Del Bo’, C, Martini, D, Bernardi, S, Gigliotti, L, Marino, M, Gargari, G, Meroño, T, Hidalgo-Liberona, N, Andres-Lacueva, C, Kroon, P, Cherubini, A, Guglielmetti, S, Porrini, M, Riso, P, Cristian Del Bo’, Daniela Martini, Stefano Bernardi, Letizia Gigliotti, Mirko Marino, Giorgio Gargari, Tomas Meroño, Nicole Hidalgo-Liberona, Cristina Andres-Lacueva, Paul A. Kroon, Antonio Cherubini, Simone Guglielmetti, Marisa Porrini, Patrizia Riso, Del Bo’, C, Martini, D, Bernardi, S, Gigliotti, L, Marino, M, Gargari, G, Meroño, T, Hidalgo-Liberona, N, Andres-Lacueva, C, Kroon, P, Cherubini, A, Guglielmetti, S, Porrini, M, Riso, P, Cristian Del Bo’, Daniela Martini, Stefano Bernardi, Letizia Gigliotti, Mirko Marino, Giorgio Gargari, Tomas Meroño, Nicole Hidalgo-Liberona, Cristina Andres-Lacueva, Paul A. Kroon, Antonio Cherubini, Simone Guglielmetti, Marisa Porrini, and Patrizia Riso

Abstract

The use of DNA damage as marker of oxidative stress, metabolic dysfunction and agerelated diseases is debated. The present study aimed at assessing the level of DNA damage (evaluated as DNA strand-breaks, endogenous and oxidatively-induced DNA damage) in a group of older subjects with intestinal permeability enrolled within the MaPLE (Gut and Blood Microbiomics for Studying the Effect of a Polyphenol-Rich Dietary Pattern on Intestinal Permeability in the Elderly) intervention trial, to evaluate its association with clinical, metabolic and dietary markers. DNA damage in peripheral blood mononuclear cells was assessed by the comet assay in 49 older subjects participating in the study. Clinical and metabolic markers, markers of inflammation, vascular function and intestinal permeability were determined in serum. Food intake was estimated by weighted food diaries. On the whole, a trend towards higher levels of DNA damage was observed in men compared to women (p = 0.071). A positive association between DNA damage and clinical/metabolic markers (e.g., uric acid, lipid profile) and an inverse association with dietary markers (e.g., vitamin C, E, B6, folates) were found and differed based on sex. By considering the importance of DNA stability during aging, the results obtained on sex differences and the potential role of dietary and metabolic factors on DNA damage underline the need for further investigations in a larger group of older adults to confirm the associations found and to promote preventive strategies.

Published
2021

19. Polyphenols and Intestinal Permeability: Rationale and Future Perspectives

Author

Bernardi, S, Del Bo’, C, Marino, M, Gargari, G, Cherubini, A, Andres-Lacueva, C, Hidalgo Liberona, N, Peron, G, González Dominguez, R, Kroon, P, Kirkup, B, Porrini, M, Guglielmetti, S, Riso, P, Stefano Bernardi, Cristian Del Bo’, Mirko Marino, Giorgio Gargari, Antonio Cherubini, Cristina Andres-Lacueva, Nicole Hidalgo Liberona, Gregorio Peron, Raúl González Dominguez, Paul Kroon, Benjamin Kirkup, Marisa Porrini, Simone Guglielmetti, Patrizia Riso, Bernardi, S, Del Bo’, C, Marino, M, Gargari, G, Cherubini, A, Andres-Lacueva, C, Hidalgo Liberona, N, Peron, G, González Dominguez, R, Kroon, P, Kirkup, B, Porrini, M, Guglielmetti, S, Riso, P, Stefano Bernardi, Cristian Del Bo’, Mirko Marino, Giorgio Gargari, Antonio Cherubini, Cristina Andres-Lacueva, Nicole Hidalgo Liberona, Gregorio Peron, Raúl González Dominguez, Paul Kroon, Benjamin Kirkup, Marisa Porrini, Simone Guglielmetti, and Patrizia Riso

Abstract

Increasing evidence links intestinal permeability (IP), a feature of the intestinal barrier, to several pathological or dysfunctional conditions. Several host and environmental factors, including dietary factors, can affect the maintenance of normal IP. In this regard, food bioactives, such as polyphenols, have been proposed as potential IP modulators, even if the mechanisms involved are not yet fully elucidated. The aim of the present paper is to provide a short overview of the main evidence from in vitro and in vivo studies supporting the role of polyphenols in modulating IP and briefly discuss future perspectives in this research area.

Published
2020

20. Effect of a polyphenol-rich dietary pattern on intestinal permeability and gut and blood microbiomics in older subjects: study protocol of the MaPLE randomised controlled trial

Author

Guglielmetti, S, Bernardi, S, Del Bo', C, Cherubini, A, Porrini, M, Gargari, G, Hidalgo-Liberona, N, Gonzalez-Dominguez, R, Peron, G, Zamora-Ros, R, Winterbone, M, Kirkup, B, Kroon, P, Andres-Lacueva, C, Riso, P, Winterbone, MS, Kroon, PA, Guglielmetti, S, Bernardi, S, Del Bo', C, Cherubini, A, Porrini, M, Gargari, G, Hidalgo-Liberona, N, Gonzalez-Dominguez, R, Peron, G, Zamora-Ros, R, Winterbone, M, Kirkup, B, Kroon, P, Andres-Lacueva, C, Riso, P, Winterbone, MS, and Kroon, PA

Abstract

Background: During aging, alterations of the intestinal microbial ecosystem can occur contributing to immunosenescence, inflamm-aging and impairment of intestinal barrier function (increased intestinal permeability; IP). In the context of a diet-microbiota-IP axis in older subjects, food bioactives such as polyphenols may play a beneficial modulatory role. Methods: MaPLE is a project centered on a randomized, controlled cross-over dietary intervention trial [polyphenol-rich diet (PR-diet) versus control diet (C-diet)] targeted to older people (≥ 60 y) living in a well-controlled setting (i.e. nursing home). The 8-week interventions are separated by an 8-week wash-out period. Three small portions per day of selected polyphenol-rich foods are consumed during intervention in substitution of other comparable products within the C-diet. Biological samples are collected before and after each treatment period to evaluate markers related to IP, inflammation, vascular function, oxidative stress, gut and blood microbiomics, metabolomics. A sample size of 50 subjects was defined based on IP as primary outcome. Discussion: Evidence that increasing the consumption of polyphenol-rich food products can positively affect intestinal microbial ecosystem resulting in reduced IP and decreased translocation of inflammogenic bacterial factors into the bloodstream will be provided. The integration of data from gut and blood microbiomics, metabolomics and other IP-related markers will improve the understanding of the beneficial effect of the intervention in the context of polyphenols-microbiota-IP interactions. Finally, findings obtained will provide a proof of concept of the reliability of the dietary intervention, also contributing to future implementations of dietary guidelines directed to IP management in the older and other at risk subjects. Trial registration: The trial is registered at (ISRCTN10214981); April 28, 2017.

Published
2020

22. Contributors

Author

Abe, C., primary, Accardi, G., additional, Andres-Lacueva, C., additional, Appendino, G., additional, Armentia, A., additional, Arora, R., additional, Azevedo, V., additional, Badole, S.L., additional, Bae, S.-C., additional, Baliga, M.S., additional, Balistreri, C.R., additional, Bermúdez-Humarán, L.G., additional, Bhat, H., additional, Bodhankar, S.L., additional, Bolling, S.F., additional, Bollor, R., additional, Bowden, R.G., additional, Bravo-Clouzet, R., additional, Calder, P.C., additional, Câmara, N.O.S., additional, Candore, G., additional, Castell, M., additional, Castellote, C., additional, Castrodeza, J., additional, Cerón, J.M., additional, Chacko, J., additional, Chowdhury, Z.T., additional, Comalada, M., additional, Contreras-Moreno, J., additional, Cordova, F.M., additional, Correa-Matos, N.J., additional, Crespo, J., additional, de Cienfuegos, G.Á., additional, de Gaetano, G., additional, de Luis, D., additional, de Moreno de LeBlanc, A., additional, de Pablo, M.A., additional, de Roos, B., additional, del Carmen, S., additional, Díaz, L.E., additional, di Giuseppe, R., additional, Donati, M.B., additional, Egger, G., additional, Elias, R.M., additional, Fayad, R., additional, Fazal, F., additional, Feleszko, W., additional, Fischer, A.K., additional, Franch, À., additional, Galena, A.E., additional, Gálvez, J., additional, Gómez-Martínez, S., additional, Graziano, C., additional, Hall, J., additional, Haniadka, R., additional, Hurst, R.D., additional, Hurst, S.M., additional, Iacoviello, L., additional, Inglada, L., additional, Jaffe, R., additional, Jaworska, J., additional, Kaufman, P.B., additional, Khan, N., additional, Kirakosyan, A., additional, Langella, P., additional, Latheef, L., additional, LeBlanc, J.G., additional, Llorach, R., additional, Lucas, E.A., additional, Malhotra, P., additional, Marcos, A., additional, Marín-Casino, M., additional, Martín-Armentia, S., additional, Mateu-de Antonio, J., additional, Menaa, A., additional, Menaa, B., additional, Menaa, F., additional, Mes, J., additional, Minato, K.I., additional, Miyoshi, A., additional, Monagas, M., additional, Moreillon, J., additional, Mullin, G.E., additional, Neyestani, T.R., additional, Oommen, B., additional, Pai, C., additional, Pai, R.J., additional, Pérez-Berezo, T., additional, Pérez-Cano, F.J., additional, Pérez de Heredia, F., additional, Petro, T.M., additional, Pozo-Rubio, T., additional, Prabhala, H.K., additional, Prabhala, R.H., additional, Pravettoni, V., additional, Prescott, S.L., additional, Primavesi, L., additional, Puertollano, E., additional, Puertollano, M.A., additional, Ramos-Romero, S., additional, Rastmanesh, R., additional, Rendina, E., additional, Romeo, J., additional, Sabetisoofyani, A., additional, Sampath, P., additional, Schauss, A.G., additional, Seymour, E.M., additional, Sharma, A., additional, Shelmadine, B., additional, Smith, B.J., additional, Somasundaram, S.G., additional, Sung, M.-K., additional, Togni, S., additional, Urpi-sarda, M., additional, Vaghefi, S.B., additional, Watson, R.R., additional, Weber, C.E., additional, West, C.E., additional, Wichers, H., additional, Wood, L.G., additional, Xaus, J., additional, Yashawanth, H.S., additional, and Zibadi, S., additional

Published
2013
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23. RED WINE POLYPHENOLS AND HUMAN HEALTH

Author

Andres-Lacueva, C., Urpi-Sarda, M., Vázquez-Fresno, R., Tulipani, S., Rotchés-Ribalta, M., Boto-Ordoñez, M., Queipo-Ortuño, M., Chiva, G., Estruch, R., Tinahones, F J., and Llorach, R.

Published
2013

26. Systematic Review on Polyphenol Intake and Health Outcomes: Is there Sufficient Evidence to Define a Health-Promoting Polyphenol-Rich Dietary Pattern?

Author

Del Bo, C., Bernardi, S., Marino, M., Porrini, M., Tucci, M., Guglielmetti, S., Cherubini, A., Carrieri, B., Kirkup, B., Kroon, P., Zamora-Ros, R., Liberona, N. H., Andres-Lacueva, C., and Riso, P.

Subjects
polyphenol databases, food and beverages, cardiovascular and all-cause mortality, Polyphenols, lcsh:TX341-641, Review, Health Promotion, disease risk, Diet, Polifenols, Chronic diseases, polyphenol intake, Chronic Disease, Malalties cròniques, Humans, dietary pattern, lcsh:Nutrition. Foods and food supply, Cardiovascular and all-cause mortality, Dietary pattern, Disease risk, Polyphenol databases, Polyphenol intake
Abstract

Growing evidence support association between polyphenol intake and reduced risk for chronic diseases, even if there is a broad debate about the effective amount of polyphenols able to exert such protective effect. The present systematic review provides an overview of the last 10-year literature on the evaluation of polyphenol intake and its association with specific disease markers and/or endpoints. An estimation of the mean total polyphenol intake has been performed despite the large heterogeneity of data reviewed. In addition, the contribution of dietary sources was considered, suggesting tea, coffee, red wine, fruit and vegetables as the main products providing polyphenols. Total flavonoids and specific subclasses, but not total polyphenols, have been apparently associated with a low risk of diabetes, cardiovascular events and all-cause mortality. However, large variability in terms of methods for the evaluation and quantification of polyphenol intake, markers and endpoints considered, makes it still difficult to establish an evidence-based reference intake for the whole class and subclass of compounds. Nevertheless, the critical mass of data available seem to strongly suggest the protective effect of a polyphenol-rich dietary pattern even if further well targeted and methodologically sound research should be encouraged in order to define specific recommendations.

Published
2019

27. Systematic Review on Polyphenol Intake and Health Outcomes: Is there Sufficient Evidence to Define a Health-Promoting Polyphenol-Rich Dietary Pattern?

Author

Del Bo’, C, Bernardi, S, Marino, M, Porrini, M, Tucci, M, Guglielmetti, S, Cherubini, A, Carrieri, C, Kirkup, B, Kroon, P, Zamora-Ros, R, Hidalgo Liberona, N, Andres-Lacueva, C, Riso, P, Del Bo’, C, Bernardi, S, Marino, M, Porrini, M, Tucci, M, Guglielmetti, S, Cherubini, A, Carrieri, C, Kirkup, B, Kroon, P, Zamora-Ros, R, Hidalgo Liberona, N, Andres-Lacueva, C, and Riso, P

Abstract

Growing evidence support association between polyphenol intake and reduced risk for chronic diseases, even if there is a broad debate about the effective amount of polyphenols able to exert such protective effect. The present systematic review provides an overview of the last 10-year literature on the evaluation of polyphenol intake and its association with specific disease markers and/or endpoints. An estimation of the mean total polyphenol intake has been performed despite the large heterogeneity of data reviewed. In addition, the contribution of dietary sources was considered, suggesting tea, coffee, red wine, fruit and vegetables as the main products providing polyphenols. Total flavonoids and specific subclasses, but not total polyphenols, have been apparently associated with a low risk of diabetes, cardiovascular events and all-cause mortality. However, large variability in terms of methods for the evaluation and quantification of polyphenol intake, markers and endpoints considered, makes it still difficult to establish an evidence-based reference intake for the whole class and subclass of compounds. Nevertheless, the critical mass of data available seem to strongly suggest the protective effect of a polyphenol-rich dietary pattern even if further well targeted and methodologically sound research should be encouraged in order to define specific recommendations.

Published
2019

28. Impact of foods and dietary supplements containing hydroxycinnamic acids on cardiometabolic biomarkers: A systematic review to explore inter-individual variability

Author

Martini, D., Chiavaroli, L., Gonzalez-Sarrias, A., Bresciani, L., Palma-Duran, S. A., Dall'Asta, Margherita, Deligiannidou, G. -E., Massaro, M., Scoditti, E., Combet, E., Maksimova, V., Urpi-Sarda, M., Kontogiorgis, C. A., Andres-Lacueva, C., Gibney, E. R., Del Rio, D., Morand, C., Garcia-Aloy, M., Rodriguez-Mateos, A., Mena, P., Dall'asta M. (ORCID:0000-0002-0558-0337), Martini, D., Chiavaroli, L., Gonzalez-Sarrias, A., Bresciani, L., Palma-Duran, S. A., Dall'Asta, Margherita, Deligiannidou, G. -E., Massaro, M., Scoditti, E., Combet, E., Maksimova, V., Urpi-Sarda, M., Kontogiorgis, C. A., Andres-Lacueva, C., Gibney, E. R., Del Rio, D., Morand, C., Garcia-Aloy, M., Rodriguez-Mateos, A., Mena, P., and Dall'asta M. (ORCID:0000-0002-0558-0337)

Abstract

Plant-based diets rich in bioactive compounds such as polyphenols have been shown to positively modulate the risk of cardiometabolic (CM) diseases. The inter-individual variability in the response to these bioactives may affect the findings. This systematic review aimed to summarize findings from existing randomized clinical trials (RCTs) evaluating the effect of hydroxycinnamic acids (HCAs) on markers of CM health in humans. Literature searches were performed in PubMed and the Web of Science. RCTs on acute and chronic supplementation of HCA-rich foods/extracts on CM biomarkers were included. Forty-four RCTs (21 acute and 23 chronic) met inclusion criteria. Comparisons were made between RCTs, including assessments based on population health status. Of the 44 RCTs, only seven performed analyses on a factor exploring inter-individual response to HCA consumption. Results demonstrated that health status is a potentially important effect modifier as RCTs with higher baseline cholesterol, blood pressure and glycaemia demonstrated greater overall effectiveness, which was also found in studies where specific subgroup analyses were performed. Thus, the effect of HCAs on CM risk factors may be greater in individuals at higher CM risk, although future studies in these populations are needed, including those on other potential determinants of inter-individual variability. PROSPERO, registration number CRD42016050790.

Published
2019

29. Non-targeted metabolomic biomarkers and metabotypes of type 2 diabetes: A cross-sectional study of PREDIMED trial participants.

Author

Universitat Rovira i Virgili, Urpi-Sarda M, Almanza-Aguilera E, Llorach R, Vázquez-Fresno R, Estruch R, Corella D, Sorli JV, Carmona F, Sanchez-Pla A, Salas-Salvadó J, Andres-Lacueva C, Universitat Rovira i Virgili, and Urpi-Sarda M, Almanza-Aguilera E, Llorach R, Vázquez-Fresno R, Estruch R, Corella D, Sorli JV, Carmona F, Sanchez-Pla A, Salas-Salvadó J, Andres-Lacueva C

Abstract

To characterize the urinary metabolomic fingerprint and multi-metabolite signature associated with type 2 diabetes (T2D), and to classify the population into metabotypes related to T2D.A metabolomics analysis using the 1H-NMR-based, non-targeted metabolomic approach was conducted to determine the urinary metabolomic fingerprint of T2D compared with non-T2D participants in the PREDIMED trial. The discriminant metabolite fingerprint was subjected to logistic regression analysis and ROC analyses to establish and to assess the multi-metabolite signature of T2D prevalence, respectively. Metabotypes associated with T2D were identified using the k-means algorithm.A total of 33 metabolites were significantly different (P<0.05) between T2D and non-T2D participants. The multi-metabolite signature of T2D comprised high levels of methylsuccinate, alanine, dimethylglycine and guanidoacetate, and reduced levels of glutamine, methylguanidine, 3-hydroxymandelate and hippurate, and had a 96.4% AUC, which was higher than the metabolites on their own and glucose. Amino-acid and carbohydrate metabolism were the main metabolic alterations in T2D, and various metabotypes were identified in the studied population. Among T2D participants, those with a metabotype of higher levels of phenylalanine, phenylacetylglutamine, p-cresol and acetoacetate had significantly higher levels of plasma glucose.The multi-metabolite signature of T2D highlights the altered metabolic fingerprint associated mainly with amino-acid, carbohydrate and microbiota metabolism. Metabotypes identified in this patient population could be related to higher risk of long-term cardiovascular events and therefore require further studies. Metabolomics is a useful tool for elucidating the metabolic complexity and interindividual va

Published
2019

30. Des dispositifs de cuisine connectés pour influencer l’homéostasie nutritionnelle : un essai contrôlé randomisé de faisabilité à domicile

Author

Vaillant, M.-F., primary, Terrisse, H., additional, Artemova, S., additional, Rolland, C., additional, Joyeux-Faure, M., additional, Borel, J.-C., additional, Marion, O., additional, Dancer, P., additional, Sicard, M., additional, Casas-Agustench, P., additional, Andres-Lacueva, C., additional, Lloyd, A.J., additional, Draper, J., additional, Pison, C., additional, and Moinard, C., additional

Published
2019
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31. FoodComEx - a chemical library for food compounds and related metabolites

Author

Manach, Claudine, Weinert, C., Pujos-Guillot, Estelle, Ulaszewska, M., Giacomoni, Franck, Mattivi, F., Urpi-Sarda, M., Andres-Lacueva, C., Kulling, S.E., Dragsted, L.O., Wishart, D., Fiamoncini, Jarlei, Unité de Nutrition Humaine (UNH), Institut National de la Recherche Agronomique (INRA)-Université Clermont Auvergne [2017-2020] (UCA [2017-2020]), Max Rubner-Institut, Centro Ricerca e Innovazione, Fondazione Edmund Mach, Instituto Agrario S. Michele all' Adige, University of Barcelona, University of Copenhagen = Københavns Universitet (KU), University of Alberta, and University of Copenhagen = Københavns Universitet (UCPH)

Subjects
[SDV]Life Sciences [q-bio], ComputingMilieux_MISCELLANEOUS
Abstract

International audience

Published
2017

33. Nutrition for the ageing brain: Towards evidence for an optimal diet

Author

Vauzour, D., Camprubi-Robles, M., Miquel-Kergoat, S., Andres-Lacueva, C., Banati, D., Barberger-Gateau, P., Bowman, G.L., Caberlotto, L., Clarke, R., Hogervorst, E., Kiliaan, A.J., Lucca, U., Manach, C., Minihane, A.M., Mitchell, E.S., Perneczky, R., Perry, H., Roussel, A.M., Schuermans, J., Sijben, J., Spencer, J.P., Thuret, S., Rest, O. van de, Vandewoude, M., Wesnes, K., Williams, R.J., Williams, R.S., Ramirez, M., Vauzour, D., Camprubi-Robles, M., Miquel-Kergoat, S., Andres-Lacueva, C., Banati, D., Barberger-Gateau, P., Bowman, G.L., Caberlotto, L., Clarke, R., Hogervorst, E., Kiliaan, A.J., Lucca, U., Manach, C., Minihane, A.M., Mitchell, E.S., Perneczky, R., Perry, H., Roussel, A.M., Schuermans, J., Sijben, J., Spencer, J.P., Thuret, S., Rest, O. van de, Vandewoude, M., Wesnes, K., Williams, R.J., Williams, R.S., and Ramirez, M.

Abstract

Contains fulltext : 174210.pdf (Publisher’s version ) (Open Access), As people age they become increasingly susceptible to chronic and extremely debilitating brain diseases. The precise cause of the neuronal degeneration underlying these disorders, and indeed normal brain ageing remains however elusive. Considering the limits of existing preventive methods, there is a desire to develop effective and safe strategies. Growing preclinical and clinical research in healthy individuals or at the early stage of cognitive decline has demonstrated the beneficial impact of nutrition on cognitive functions. The present review is the most recent in a series produced by the Nutrition and Mental Performance Task Force under the auspice of the International Life Sciences Institute Europe (ILSI Europe). The latest scientific advances specific to how dietary nutrients and non-nutrient may affect cognitive ageing are presented. Furthermore, several key points related to mechanisms contributing to brain ageing, pathological conditions affecting brain function, and brain biomarkers are also discussed. Overall, findings are inconsistent and fragmented and more research is warranted to determine the underlying mechanisms and to establish dose-response relationships for optimal brain maintenance in different population subgroups. Such approaches are likely to provide the necessary evidence to develop research portfolios that will inform about new dietary recommendations on how to prevent cognitive decline.

Published
2017

34. Clinical phenotype clustering in cardiovascular risk patients for the identification of responsive metabotypes after red wine polyphenol intake

Author

Vázquez-Fresno R, Llorach R, Perera A, Mandal R, Feliz M, Tinahones FJ, Wishart DS, and Andres-Lacueva C

Subjects
4-Hydroxyphenylacetate, Cardiovascular disease, Gut microbiota, Metabolic phenotype, Metabolomics, Metabotype, NMR, Wine polyphenols
Abstract

This study aims to evaluate the robustness of clinical and metabolic phenotyping through, for the first time, the identification of differential responsiveness to dietary strategies in the improvement of cardiometabolic risk conditions. Clinical phenotyping of 57 volunteers with cardiovascular risk factors was achieved using k-means cluster analysis based on 69 biochemical and anthropometric parameters. Cluster validation based on Dunn and Figure of Merit analysis for internal coherence and external homogeneity were employed. k-Means produced four clusters with particular clinical profiles. Differences on urine metabolomic profiles among clinical phenotypes were explored and validated by multivariate orthogonal signal correction partial least-squares discriminant analysis (OSC-PLS-DA) models. OSC-PLS-DA of (1)H-NMR data revealed that model comparing "obese and diabetic cluster" (OD-c) against "healthier cluster" (H-c) showed the best predictability and robustness in terms of explaining the pairwise differences between clusters. Considering these two clusters, distinct groups of metabolites were observed following an intervention with wine polyphenol intake (WPI; 733 equivalents of gallic acid/day) per 28days. Glucose was significantly linked to OD-c metabotype (P

Published
2016

35. FoodComEx: une chimiothèque internationale pour les composés dérivés de l’alimentation

Author

Wishart, D., Weinert, C., Pujos-Guillot, Estelle, Ulaszewska, M., Giacomoni, Franck, Mattivi, F., Urpi-Sarda, M., Andres-Lacueva, C., Kulling, S.E., Dragsted, L.O., Manach, Claudine, University of Alberta, Max Rubner-Institut, Unité de Nutrition Humaine (UNH), Institut National de la Recherche Agronomique (INRA)-Université d'Auvergne - Clermont-Ferrand I (UdA)-Clermont Université, Centro Ricerca e Innovazione, Fondazione Edmund Mach, Instituto Agrario S. Michele all' Adige, University of Barcelona, University of Copenhagen = Københavns Universitet (UCPH), Projet FoodBall JPI HDHL, Centre de Recherche en Nutrition Humaine (CRNH). FRA., and University of Copenhagen = Københavns Universitet (KU)

Subjects
projet européen, alimentation, chimiotheque, composé, composé dérivé de l’alimentation, Alimentation et Nutrition, Food and Nutrition, [SDV.AEN]Life Sciences [q-bio]/Food and Nutrition
Abstract

National audience; Le manque de standards commerciaux pour de nombreux composés dérivés de l’alimentation, en particulier les métabolites retrouvés dans le sang et les tissus chez l’homme après consommation des aliments constitue une limitation importante en nutrition. Par exemple l’identification de centaines de métabolites détectés dans les profils métabolomiques reste difficile sans standard, d’autre part les études mécanistiques sur modèles cellulaires se font encore trop souvent avec des composés qui ne sont pas ceux retrouvés au niveau physiologique. FoodComEx (Food Compound Exchange, http://foodcomex.org/) est une nouvelle chimiothèque initiée dans le cadre du projet européen FoodBAll pour faciliter l’accès à des molécules dérivées de l’alimentation qui sont aujourd’hui peu ou pas disponibles. Dans le cadre de projets divers, beaucoup de composés ont été produits à petite échelle dans des laboratoires académiques, par synthèse chimique ou enzymatique, par purification à partir de matrices biologiques ou encore par incubation avec des microorganismes. Des collections entières de composés précieux dorment dans des laboratoires du monde entier. L’objectif de FoodComEx est de mettre à disposition ces composés pour une large communauté d’utilisateurs. FoodComEx sera un catalogue interrogeable en ligne des composés disponibles, indiquant les coordonnées du laboratoire offrant de partager chaque composé. Tout utilisateur intéressé contactera directement le laboratoire producteur et les termes de la collaboration seront décidés par les deux partenaires, dans le cadre de la charte des bonnes pratiques de FoodComEx. Des données physico-chimiques, spectrales ainsi que des informations décrivant l’origine du composé, sa stabilité, sa pureté, etc seront disponibles dans la fiche de chaque composé. Les données analytiques seront enrichies continuellement par les utilisateurs. FoodComEx est une initiative récente qui bénéficie déjà du soutien de réseaux tels que la société allemande des food chemists et l’action COST POSITIVe. Tout laboratoire souhaitant partager des composés dérivés de l’alimentation est évidemment le bienvenu pour enrichir la collection de FoodComEx et permettre de nouvelles collaborations. Financement : Projet FoodBall JPI HDHL.

Published
2015

37. FoodComEx, a new chemical library for rare food-derived compounds

Author

Weinert, C., Ulaszewska, M., Pujos-Guillot, E., Sajed, T., Vazquez-Fresno, R., Remus Rosana, A., Mattivi, F., Giacomini, F., Urpi-Sarda, M., Andres-Lacueva, C., Kulling, S., Wishart, D., and Manach, C.

Subjects
Settore CHIM/10 - CHIMICA DEGLI ALIMENTI
Published
2015

39. Markers of inflammation, Vitamin E and peripheral nervous system function The InCHIANTI study

Author

Di Iorio A., Cherubini A., Volpato S., Sparvieri E., Lauretani F., Senin U., Abate G., Paganelli R., Martin A., Andres Lacueva C., Ferrucci L., FRANCESCHI, CLAUDIO, Di Iorio A., Cherubini A., Volpato S., Sparvieri E., Lauretani F., Franceschi C., Senin U., Abate G., Paganelli R., Martin A., Andres-Lacueva C., and Ferrucci L.

Subjects
Inflammation, Aging, Vitamin E, Peripheral nervous system
Published
2006

41. Nutrimetabolomics fingerprinting to identify biomarkers of bread exposure in a free-living population from the PREDIMED study cohort

Author

Bioquímica i Biotecnologia, Universitat Rovira i Virgili, Garcia-Aloy, M; Llorach, R; Urpi-Sarda, M; Tulipani, S; Salas-Salvado, J; Martinez-Gonzalez, MA; Corella, D; Fito, M; Estruch, R; Serra-Majem, L; Andres-Lacueva, C, Bioquímica i Biotecnologia, Universitat Rovira i Virgili, and Garcia-Aloy, M; Llorach, R; Urpi-Sarda, M; Tulipani, S; Salas-Salvado, J; Martinez-Gonzalez, MA; Corella, D; Fito, M; Estruch, R; Serra-Majem, L; Andres-Lacueva, C

Published
2015

42. Metabolomics for Biomarkers of Type 2 Diabetes Mellitus: Advances and Nutritional Intervention Trends

Author

Universitat Rovira i Virgili, Urpi-Sarda M; Almanza-Aguilera E; Tulipani S; Tinahones F; Salas-Salvadó J; Andres-Lacueva C, Universitat Rovira i Virgili, and Urpi-Sarda M; Almanza-Aguilera E; Tulipani S; Tinahones F; Salas-Salvadó J; Andres-Lacueva C

Abstract

Metabolic characterization of type 2 diabetes mellitus (T2DM) is crucial for the identification of individuals at risk for developing diabetes and T2DM-related vascular complications as well as for monitoring disease progression. The application of metabolomics to diabetes research may lead to the identification and discovery of diagnostic and prognostic T2DM biomarkers, in addition to elucidating disease pathways. In the present review, we summarize the distinct classes of metabolites that have been proposed as potential biomarkers for progressing stages of T2DM by metabolomic approaches. Several studies have demonstrated that the metabolism of carbohydrates, lipids, and amino acids is considerably altered in prediabetes and continue to vary over the course of T2DM progression. The identification of intermediate metabolites involved in glycolysis, gluconeogenesis, the tricarboxylic acid cycle, lipolysis, and proteolysis have provided evidence of these metabolic dysfunctions. Finally, given the increasing worldwide incidence of T2DM and its related complications, research should focus on the impact of lifestyle factors, particularly diet, at the metabolomic level for better understanding and improved healthcare strategies.

Published
2015

43. Exploiting the phenol-explorer 2.0 database to analyze and characterize the polyphenol metabolome

Author

Rothwell, J.A, Urpi-Sarda, M., Boto-Ordonez, M., Llorach, R., Kumar, D., Neveu, V., Manach, Claudine, Andres-Lacueva, C., Scalbert, A, Nutrition and Metabolism Section, Biomarkers Group, International Agency for Cancer Research (IACR), Institut d'Investigació Biomèdica August Pi i Sunyer, Department of Internal Medicine, University of Barcelona, CIBER 08/08 : Fisiopatología de la Obesidad y la Nutrición and RD06/0045/1003 Alimentación Saludable, Instituto de Salud Carlos III (ISC), Pharmacy Faculty, Nutrition and Food Science Department, Ingenio - CONSOLIDER program, FUN - C - FOOD, Unité de Nutrition Humaine (UNH), Clermont Université-Université d'Auvergne - Clermont-Ferrand I (UdA)-Institut National de la Recherche Agronomique (INRA), FUN - C – FOOD, Danone Research, French National Institute of Cancer, University of Barcelona, Instituto de Salud Carlos III [Madrid] (ISC), Institut National de la Recherche Agronomique (INRA)-Université d'Auvergne - Clermont-Ferrand I (UdA)-Clermont Université, and Centre de Recherche en Nutrition Humaine (CRNH). FRA.

Subjects
polyphénol, base de données en ligne, Alimentation et Nutrition, food and beverages, Food and Nutrition, [SDV.AEN]Life Sciences [q-bio]/Food and Nutrition, profil métabolique
Abstract

Presenting author: J.A. Rothwell We gratefully acknowledge Danone Research, the French National Institute of Cancer and the University of Barcelona for financing the project.Presenting author: J.A. Rothwell We gratefully acknowledge Danone Research, the French National Institute of Cancer and the University of Barcelona for financing the project.; Phenol-Explorer is an open-access web database on polyphenols, a major group ofphytochemicals abundant in plant foods. Version 2.0 of the database was released in late 2011 andincludes comprehensive qualitative and quantitative data on the ‘polyphenol metabolome’ (i.e. allmetabolites derived from the over 500 polyphenols known in foods) in humans and experimentalanimals. Such databases are necessary for the screening of metabolomic profiles and theidentification of potential biomarkers of food consumption. The aim of this study was to analysethese new data to characterize and visualize the polyphenol metabolome. The update wasimplemented by the compilation of data on 383 polyphenol metabolites from 221 originalintervention studies. Research articles were first screened for suitability using pre-defined criteriaand then entered into a relational database via Microsoft Access. The polyphenol metabolome wasthen analyzed via a series of database queries and open-source visualization software. Data weremainly obtained in human and rat models, and profiles of metabolites were similar between thesespecies. The highest Cmax values (maximum plasma concentration) were found in rats, as higherdoses of pure polyphenols could be administered, although in both species, administration of purepolyphenols or polyphenol supplements led to much higher plasma concentrations thanadministration of foods. Conversely, Tmax (time to reach Cmax) was species-dependent and alwaysshorter in the rat. Additionally, the ensemble of all studies administering pure compounds to humansand animals allowed an insight into precursor-metabolite specificity. 5-O-Caffeoylquinic acid,catechin and epicatechin gave rise to the broadest range of metabolites, while hippuric, ferulic, 4-hydroxybenzoic, dihydrocaffeic and vanillic acids were the metabolites derived from the largestnumber of precursors. Knowledge of polyphenol metabolism is crucial to understanding their in vivobioactivities and the polyphenol metabolome is an important component of the information-richfood metabolome, which encompasses all metabolites derived from exposure to the diet.We gratefully acknowledge Danone Research, the French National Institute of Cancer and theUniversity of Barcelona for financing the project.

Published
2013

44. Resveratrol administration or SIRT1 overexpression does not increase LXR signaling and macrophage-to-feces reverse cholesterol transport in vivo

Author

Escolà-Gil J.C., Julve J., Llaverias G., Urpi-Sarda M., Silvennoinen R., Lee-Rueckert M., Andres-Lacueva C., and Blanco-Vaca F.

Subjects
insulin, lipid absorption, gene overexpression, animal experiment, dihydroresveratrol sulfoglucuronide, cholesterol blood level, resveratrol sulfoglucuronide, insulin blood level, animal cell, macrophage, resveratrol, sirtuin 1, cholesterol liver level, animal tissue, gene targeting, resveratrol 3,4 o disulfate, in vivo study, male, radioact, cholesterol transport, dihydroresveratrol, transcription factor FKHR, controlled study, isotope labeling, glucose, n (2,2,2 trifluoroethyl) n [4 [2,2,2 trifluoro 1 hydroxy 1 (trifluoromethoxy)ethyl]phenyl]benzenesulfonamide, mouse, dihydroresveratrol sulfate, dihydroresveratrol glucuronide 1, hydroxymethylglutaryl coenzyme A reductase, nonhuman, dihydroresveratrol glucuronide 2, article, cholesterol, cholesterol 7alpha monooxygenase, resveratrol 4' o glucuronide, unclassified drug, female, glucose blood level, feces, priority journal, drug blood level, resveratrol 4' o sulfate, resveratrol 3 o sulfate, resveratrol 3 o glucuronide, liver X receptor
Abstract

The natural polyphenol resveratrol has cardiometabolic protective properties. Resveratrol has been reported to be an activator of NAD +-dependent deacetylase sirtuin 1 (SIRT1), which may regulate liver X receptor (LXR) activity, thereby upregulating the expression of genes crucial in reverse cholesterol transport (RCT). In the present study, the effects of resveratrol and SIRT1 overexpression on RCT from macrophages-to-feces in vivo in C57BL/6 mice were determined. [3H]cholesterol-labeled mouse macrophages were injected intraperitoneally into mice treated with intragastric doses of the well-known LXR agonist T0901317, resveratrol, or a vehicle solution, and radioactivity was determined in plasma, liver, and feces. T0901317-treated mice presented increased [3H]cholesterol in plasma and HDL 48 h after the label injection. Treatment with T0901317 also increased liver ABCA1, G1, and G5 gene expression and reduced intestinal cholesterol absorption which were changes that were associated with a 2.8-fold increase in macrophage-derived [3H]cholesterol in feces. In contrast, resveratrol treatment had no effect on liver LXR signaling or fecal [3H] cholesterol excretion. A separate experiment was conducted in SIRT1 transgenic mice. Liver LXR-target gene expression and magnitude of macrophage-derived [3H]cholesterol in plasma, liver, and feces of SIRT1 transgenic mice did not differ from those of wild-type mice. We conclude that neither resveratrol administration nor SIRT1 overexpression upregulate liver LXR-target genes and macrophage-to-feces RCT in vivo. © 2013 Mosby, Inc. All rights reserved.

Published
2013

45. Cocoa consumption reduces NF-kappa B activation in peripheral blood mononuclear cells in humans

Author

Vazquez-Agell, M, Urpi-Sarda, M, Sacanella, E, Camino-Lopez, S, Chiva-Blanch, G, Llorente-Cortes, V, Tobias, E, Roura, E, Andres-Lacueva, C, Lamuela-Raventos, RM, Badimon, L, and Estruch, R

Subjects
Cocoa powder, Inflammation, NF-kappa B, Polyphenols, Adhesion molecules, Matrix effect
Abstract

Background and aims: Epidemiological studies have demonstrated an association between high-polyphenol intake and reduced incidence of atherosclerosis. The healthy effects of cocoa-polyphenols may be due to their antioxidant and anti-inflammatory actions, although the exact mechanisms are unknown and depend on the matrix in which cocoa-polyphenols are delivered. Nuclear factor kappa B (NF-kappa B) is a key molecule in the pathophysiology of atherosclerosis involved in the regulation of adhesion molecules(AM) and cytokine expression and its activation is the first step in triggering the inflammatory process. The aim of this study was to evaluate the effect of acute cocoa consumption in different matrices related to the bioavailability of cocoa-polyphenols in NF-kappa B activation and the expression of AM. Methods and results: Eighteen healthy volunteers randomly received 3 interventions: 40g of cocoa powder with milk (CM), with water (CW), and only milk (M). NF-kappa B activation in leukocytes and AM (sICAM, sVCAM, E-selectin) were measured before and 6h after each intervention. Consumption of CW significantly decreased NF-kappa B activation compared to baseline and to CM (P < 0.05, both), did not change after CM intervention, and significantly increased after M intervention (P = 0.014). sICAM-1 concentrations significantly decreased after 6h of CW and CM interventions (P

Published
2013

48. Omega-3 polyunsaturated fatty acids and immune-mediated diseases: inflammatory bowel disease and rheumatoid arthritis

Author

Ruggiero, Carmelinda, Lattanzio, F, Lauretani, F, Gasperini, Beatrice, ANDRES LACUEVA, C, and Cherubini, Antonio

Subjects
Arthritis, Rheumatoid, Fish Oils, Dietary Supplements, Fatty Acids, Omega-3, Humans, Inflammatory Bowel Diseases
Abstract

Inflammation is part of the normal host response to infection and injury. However, inappropriate inflammation contributes to several diseases, including inflammatory bowel disease (IBD) and rheumatoid arthritis (RA). Both conditions are characterized by the excessive production of inflammatory cytokines, arachidonic acid (AA)-derived eicosanoids, and other inflammatory agents (e.g., reactive oxygen species, adhesion molecules). By virtue of their anti-inflammatory action, omega-3 polyunsaturated fatty acids (PUFA) may be beneficial in inflammatory diseases. A large body of evidence supports a protective effect of omega-3 PUFA in experimental animal and ex-vivo models of Crohn's disease (CD), Ulcerative colitis (UC) and Rheumatoid arthritis (RA). Although fish oil supplementation in patients with IBD results in omega-3 PUFA incorporation into gut mucosal tissue and modification of inflammatory mediator profiles, the evidence of clinical benefits of omega-3 PUFA is weak. On the other hand, more convincing data support the efficacy of omega-3 PUFA in reducing pain, number of tender joints, duration of morning stiffness, use of non-steroidal anti-inflammatory drugs and improving physical performance in RA patients. In both IBD and RA further clinical trials with large sample size are needed to clarify the efficacy of omega-3 PUFA as a treatment.

Published
2010

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