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1. Antioxidant and free radical scavenging effects in extracts of the medicinal herb Achyrocline satureioides (Lam.) DC. ('marcela')

Author

Desmarchelier C., Coussio J., and Ciccia G.

Subjects
Achyrocline satureioides, antioxidant activity, luminol-enhanced chemiluminescence, thiobarbituric acid-reactive substances, hydroperoxide-initiated chemiluminescence, lipid peroxidation, DNA damage, reactive oxygen species, Medicine (General), R5-920, Biology (General), QH301-705.5
Abstract

Achyrocline satureioides (Lam.) DC. (Compositae) is a medicinal herb used in Argentina, Uruguay, Brazil and Paraguay for its choleretic, antispasmodic and hepatoprotective properties. The presence of the flavonoid quercetin and its derivatives, and of different phenolic acids such as caffeic, chlorogenic and isochlorogenic acids in the aerial parts of this plant has led us to study the antioxidant activity of its extracts using different bioassays. The inhibition of luminol-enhanced chemiluminescence by the aqueous and methanolic extracts was used to show that their total reactive antioxidant potential index (TRAP; in µM Trolox equivalents) was 91.0 ± 15.4 and 128.1 ± 20.1 µM, respectively, while the total antioxidant reactivity index (TAR) was calculated to be 1537 ± 148 and 1910 ± 171 µM. Only the methanolic extract was capable of reducing iron (II)-dependent DNA damage. Lipid peroxidation was assessed by two different methods. The aqueous extract reduced hydroperoxide-initiated chemiluminescence in rat liver homogenates at all concentrations in a dose-dependent manner, with a calculated IC50 = 225 µg/ml, while the methanolic extract was only effective at higher concentrations (100 and 1000 µg/ml). Both aqueous and methanolic extracts were capable of reducing the production of thiobarbituric acid reactive substances (TBARS) in rat liver homogenates, with an IC50 >1000 µg/ml. The results obtained suggest that the extracts of A. satureioides possess significant free radical scavenging and antioxidant activity in vitro, a fact that should encourage future in vivo studies.

Published
1998

5. Symposium 2: Nutrient interactions and their role in protection from chronic diseases: ß-Carotene in the human body: Metabolic bioactivation pathways - From digestion to tissue distribution and excretion

Author

Bohn T., Desmarchelier C., El S.N., Keijer J., Van Schothorst E., Rühl R., Borel P., and Ege Üniversitesi

Subjects
Micellisation, Apo-carotenoids, Retinoic acid, Nuclear hormone receptor, Vitamin A, Absorption, SNPs
Abstract

EgeUn###, ß-Carotene intake and tissue/blood concentrations have been associated with reduced incidence of several chronic diseases. Further bioactive carotenoid-metabolites can modulate the expression of specific genes mainly via the nuclear hormone receptors: retinoic acid receptor- and retinoid X receptor-mediated signalling. To better understand the metabolic conversion of ß-carotene, inter-individual differences regarding ß-carotene bioavailability and bioactivity are key steps that determine its further metabolism and bioactivation and mediated signalling. Major carotenoid metabolites, the retinoids, can be stored as esters or further oxidised and excreted via phase 2 metabolism pathways. In this review, we aim to highlight the major critical control points that determine the fate of ß-carotene in the human body, with a special emphasis on ß-carotene oxygenase 1. The hypothesis that higher dietary ß-carotene intake and serum level results in higher ß-carotene-mediated signalling is partly questioned. Alternative autoregulatory mechanisms in ß-carotene / retinoid-mediated signalling are highlighted to better predict and optimise nutritional strategies involving ß-carotene-related health beneficial mediated effects. © 2019 The Authors.

Published
2019

36. Total Reactive Antioxidant Potential (TRAP) and Total Antioxidant Reactivity (TAR) of Medicinal Plants Used in Southwest Amazonia (Bolivia and Peru)

Author

Desmarchelier, C, Repetto, M, Coussio, J, Llesuy, S, and Ciccia, G

Abstract

The charge (relative concentration) of antioxidants in different extracts of medicinal plants used in southwest Amazonia regions of Beni (Bolivia) and Madre de Dios (Peru) was determined employing a procedure based on the quenching of luminol-enhanced chemiluminescence derived from the thermolysis of 2,2'-azo- bis (2-amidinopropane) (ABAP) as the free radical source. Total reactive antioxidant potential (TRAP) and total antioxidant reactivity (TAR) values were determined (in Trolox equivalents) using this method, and 65 extracts showed antioxidant activity. Of these, 46 demonstrated TRAP values > 100 µM. The highest activity was noted in a methanol bark extract of Copaifera reticulata (TRAP = 7500 µM). On the other hand, the highest TAR value was obtained in the methanol root extract of Dracontium loretense. IC 50 and eficiency (compared to Trolox) values were also calculated. The results obtained indicate that the large antioxidant capacity of some medicinal plants may be due to the presence of both very reactive and low reactive antioxidants, the later in rather high concentrations, and that the therapeutic action claimed for some of these plants could be due, in part, to their capacity for scavenging oxygen free radicals which are involved in many diseases. The use of luminol-enhanced chemiluminescence proved to be a simple, sensitive and reproducible method that can be used to determine the antioxidant capacity in complex mixtures such as plant extracts.

Published
1997
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37. Antioxidant and Prooxidant Activities in Aqueous Extracts of Argentine Plants

Author

Desmarchelier, C., Novoa Bermudez, M.J., Coussio, J., Ciccia, G., and Boveris, A.

Abstract

The antioxidant and prooxidant activities of lyophilized aqueous extracts of 19 Argentine plants were studied using the hydroperoxide-initiated chemiluminescence assay in liver homogenates. Six extracts were found to have an effective antioxidant activity in the range 10–1000 µg dry weight/ml and were further evaluated using the thiobarbituric acid assay (TBARS). Acanthospermum australe, Baccharis coridifolia and B. crispa showed the higher antioxidant activity with both assay systems. Eleven extracts showed antioxidant activity when added in higher amounts and prooxidant activity at lower amounts. Two extracts, from Baccharis grisebachii and Terminalia triflora exhibited prooxidant activity in the 10–1000 µg range.

Published
1997
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41. Extracts of Bolivian plants, Copaifera reticulataand Heisteria pallidainhibit in vitrofree radical‐mediated DNA damage

Author

Desmarchelier, C., Coussio, J., and Ciccia, G.

Abstract

The presence of different extracts of antiinflammatory plants Copaifera reticulataand Heisteria pallidain a reaction medium containing calf thymus DNA in a free radical generating system protected DNA against oxidative damage in terms of deoxyribose oxidation. The highest antioxidant activity was obtained using the methanol extract of C. reticulata(IC50=3 μg/mL), followed by the aqueous extracts of H. pallida(IC50=257 μg/mL) and C. reticulata(IC50=380 μg/mL). Both dichloromethane extracts and the methanol extract of H. pallidashowed a decreased antioxidant activity at higher concentrations. These results suggest that these extracts are capable of suppressing the in vitrooxidative degradation of DNA. © 1997 John Wiley & Sons, Ltd.

Published
1997
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42. Evaluation of the in vitroantioxidant activity in extracts of Uncaria tomentosa(Willd.) DC.

Author

Desmarchelier, C., Mongelli, E., Coussio, J., and Ciccia, G.

Abstract

Different extracts of U. tomentosawere tested in vitrofor their antioxidant activity utilizing tert‐butyl‐hydroperoxide‐initiated chemiluminescence in rat liver homogenates. Methanol fractions of both stem‐bark and roots were capable of exerting antioxidant activity by this technique. The presence of different concentrations of bark and root methanol extracts also prevented TBARS production and free radical‐mediated DNA‐sugar damage. © 1997 John Wiley & Sons, Ltd.

Published
1997
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43. C57Bl/6 N mice on a western diet display reduced intestinal and hepatic cholesterol levels despite a plasma hypercholesterolemia

Author

Desmarchelier Charles, Dahlhoff Christoph, Keller Sylvia, Sailer Manuela, Jahreis Gerhard, and Daniel Hannelore

Subjects
Biotechnology, TP248.13-248.65, Genetics, QH426-470
Abstract

Abstract Background Small intestine and liver greatly contribute to whole body lipid, cholesterol and phospholipid metabolism but to which extent cholesterol and phospholipid handling in these tissues is affected by high fat Western-style obesogenic diets remains to be determined. Methods We therefore measured cholesterol and phospholipid concentration in intestine and liver and quantified fecal neutral sterol and bile acid excretion in C57Bl/6 N mice fed for 12 weeks either a cholesterol-free high carbohydrate control diet or a high fat Western diet containing 0.03% (w/w) cholesterol. To identify the underlying mechanisms of dietary adaptations in intestine and liver, changes in gene expression were assessed by microarray and qPCR profiling, respectively. Results Mice on Western diet showed increased plasma cholesterol levels, associated with the higher dietary cholesterol supply, yet, significantly reduced cholesterol levels were found in intestine and liver. Transcript profiling revealed evidence that expression of numerous genes involved in cholesterol synthesis and uptake via LDL, but also in phospholipid metabolism, underwent compensatory regulations in both tissues. Alterations in glycerophospholipid metabolism were confirmed at the metabolite level by phospolipid profiling via mass spectrometry. Conclusions Our findings suggest that intestine and liver react to a high dietary fat intake by an activation of de novo cholesterol synthesis and other cholesterol-saving mechanisms, as well as with major changes in phospholipid metabolism, to accommodate to the fat load.

Published
2012
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44. Identification of Genetic Polymorphisms Associated with Interindividual Variability of Vitamin A Concentration in Adipose Tissue of Healthy Male Adults.

Author

Zumaraga MP, Desmarchelier C, Gleize B, Nowicki M, Ould-Ali D, Landrier JF, and Borel P

Abstract

Background: Adipose tissue vitamin A (VA), that is, mainly retinol (RET) and its esters, comes from preformed VA and proVA carotenoids present in our food. Adipose tissue VA acts as hormonal cue maintaining essential aspects of adipocyte biology, which includes fat mobilization and catabolism, energy balance, and glucose homeostasis, and it is thus of particular interest to study its determinants, including genetic ones., Objectives: This study aimed to identify genetic variations associated with adipose tissue VA concentration., Methods: Forty-two healthy male adults received, in a randomized crossover design, 3 test meals. Periumbilical adipose tissue samples were collected on 6 occasions, that is, at fast and 8 h after consumption of each meal. RET concentration was measured in both plasma and the adipose tissue following saponification. Participants were genotyped using whole-genome microarrays. A total of 1305 single nucleotide polymorphism (SNPs) in or near 27 candidate genes were included for univariate analysis. Partial least squares (PLS) regression was carried out to find the best combination of SNPs associated with the interindividual variability in adipose tissue RET concentration., Results: Adipose tissue RET concentration was not associated with plasma RET concentrations (r = -0.184, P = 0.28). Interindividual variability of adipose tissue RET concentration was high (CV = 62%). Twenty-nine SNPs were significantly (P < 0.05) associated with adipose tissue RET concentration and a PLS regression model identified 16 SNPs as explanatory variables of this concentration. The SNPs were in or near peroxisome proliferator activated receptor gamma, retinoid X receptor alpha, signaling receptor and transporter of retinol, cluster of differentiation 36, free fatty acid receptor 4, aldehyde dehydrogenase 1 family member A1, monoglyceride lipase, DGAT2, and polycystic kidney disease 1-like 2., Conclusions: A combination of 16 SNPs has been associated with the interindividual of adipose tissue VA concentration in humans. This trial was registered at clinicaltrials.gov as NCT02100774., Competing Interests: Conflict of interest PB reports financial support provided by European Commission. All other authors report no conflicts of interest., (Copyright © 2024. Published by Elsevier Inc.)

Published
2024
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45. Characterization of the interindividual variability of lutein and zeaxanthin concentrations in the adipose tissue of healthy male adults and identification of combinations of genetic variants associated with it.

Author

Zumaraga MP, Desmarchelier C, Gleize B, Nowicki M, Ould-Ali D, and Borel P

Subjects
Humans, Male, Adult, Middle Aged, Young Adult, Genotype, Polymorphism, Single Nucleotide, Zeaxanthins metabolism, Lutein metabolism, Adipose Tissue metabolism
Abstract

Lutein (L) and zeaxanthin (Z) are involved in visual function and could prevent age-related macular degeneration and chronic diseases and improve cognitive performances. Adipose tissue is the main storage site for these xanthophylls (Xanth). The factors affecting their concentrations in this tissue remain poorly understood but in animal models, genetic variations in apolipoprotein E and β-carotene oxygenase 2 have been associated with adipose tissue L concentration. Therefore, the aims of this study were to better characterize the interindividual variability of adipose tissue Xanth concentration and to identify single nucleotide polymorphisms (SNPs) associated with it. Periumbilical subcutaneous adipose tissue samples were collected on 6 occasions in 42 healthy adult males and L and Z concentrations were measured by HPLC. Participants had their whole genome genotyped and the associations of 3589 SNPs in 49 candidate genes with the concentrations of L and Z were measured. Mean L and Z concentrations were 281 ± 27 and 150 ± 14 nmol g -1 proteins, respectively. There was no significant correlation between plasma and adipose tissue Xanth concentrations, although the correlation for L approached significance (Pearson's r = 0.276, p = 0.077). Following univariate filtering, 109 and 97 SNPs were then entered into a partial least squares regression analysis to identify the combination of SNPs that explained best adipose tissue concentration of L and Z, respectively. A combination of 7 SNPs in ELOVL5 , PPARG , ISX and ABCA1 , explained 58% of the variability in adipose tissue L concentration while 11 SNPs located in or near PPARG , ABCA1 , ELOVL5 , CXCL8 , IRS1 , ISX , MC4R explained 53% of the variance in adipose tissue Z concentration. This suggests that some genetic variations influence the concentrations of these Xanth in adipose tissue and could therefore indirectly influence the health effects of these compounds. Clinical Trial Registry: https://ClinicalTrials.gov registration number NCT02100774.

Published
2024
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46. Genetic Factors Contributing to Interindividual Variability of α-Tocopherol Levels in Subcutaneous Adipose Tissue among Healthy Adult Males.

Author

Zumaraga MP, Borel P, Gleize B, Nowicki M, Ould-Ali D, Landrier JF, and Desmarchelier C

Subjects
Humans, Male, Adult, Young Adult, Fasting, ATP Binding Cassette Transporter 1 genetics, ATP Binding Cassette Transporter 1 metabolism, CD36 Antigens genetics, CD36 Antigens metabolism, Healthy Volunteers, alpha-Tocopherol blood, alpha-Tocopherol metabolism, Polymorphism, Single Nucleotide, Subcutaneous Fat metabolism, Cross-Over Studies
Abstract

In humans, α-tocopherol (α-TOC) is mainly stored in adipose tissue, where it participates in preventing damages induced by inflammation and reactive oxygen species. Factors, including genetic ones, that explain adipose tissue α-TOC concentration remain poorly understood. This study, therefore, aimed to characterize the interindividual variability of adipose tissue α-TOC concentration in healthy individuals and to identify single nucleotide polymorphisms (SNPs) associated with it. The study used a randomized cross-over design with 42 healthy adult males. α-TOC concentration was measured in fasting plasma and periumbilical adipose tissue samples, both at fast and 8 h after consumption of three standard meals. Partial least squares (PLS) regression was performed to identify SNPs associated with the interindividual variability of adipose tissue α-TOC concentration. Adipose tissue α-TOC concentration was not associated with fasting plasma concentration (Pearson's r = 0.24, 95% CI: [-0.08, 0.51]). There was a high interindividual variability of adipose tissue α-TOC concentration (CV = 61%). A PLS regression model comprising 10 SNPs in five genes ( PPARG , ABCA1 , BUD13 , CD36 , and MGLL ) explained 60% (adjusted R 2 ) of the variability of this concentration. The interindividual variability of adipose tissue α-TOC concentration in humans is due, at least partly, to SNPs in genes involved in α-TOC and triglyceride metabolism.

Published
2024
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47. Fatty acid/monoglyceride type and amount modulate fat-soluble vitamin absorption from mixed assemblies in mice.

Author

El Aoud A, Marze S, Halimi C, Desmarchelier C, Vairo D, and Reboul E

Subjects
Mice, Animals, gamma-Tocopherol, Retinyl Esters pharmacology, Micelles, Intestinal Absorption, Vitamins, Vitamin A metabolism, Cholecalciferol, Oleic Acid, Monoglycerides, Fatty Acids pharmacology, Caprylates, Glycerides
Abstract

We investigated the effects of fatty acid/ monoglyceride type and amount on the absorption of fat-soluble vitamins. Micelles or vesicles made with either caprylic acid (CA) + monocaprylin (MC) or oleic acid (OA) + monoolein (MO) at low or high concentrations were infused in bile duct-ligated mice. Retinol + retinyl ester and γ-tocopherol intestinal mucosa contents were higher in mice infused with CA + MC than with OA + MO (up to + 350 % for vitamin A and up to + 62 %, for vitamin E; p < 0.05). Cholecalciferol intestinal mucosa content was the highest in mice infused with micelles with CA + MC at 5 mg/mL (up to + 105 %, p < 0.05). Retinyl ester plasma response was higher with mixed assemblies formed at low concentration of FA + MG compared to high concentration (up to + 1212 %, p < 0.05), while no difference in cholecalciferol and γ-tocopherol plasma responses were measured. No correlation between size or zeta potential and vitamin absorption was found. The impact of FA and MG on fat-soluble vitamin absorption thus differs from one vitamin to another and should be considered to formulate adequate vitamin oral or enteral supplements., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published
2024
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48. Effect of tomato, tomato-derived products and lycopene on metabolic inflammation: from epidemiological data to molecular mechanisms.

Author

Landrier JF, Breniere T, Sani L, Desmarchelier C, Mounien L, and Borel P

Abstract

The goal of this narrative review is to summarise the current knowledge and limitations related to the anti-inflammatory effects of tomato, tomato-derived products and lycopene in the context of metabolic inflammation associated to cardiometabolic diseases. The potential of tomato and tomato-derived product supplementation is supported by animal and in vitro studies. In addition, intervention studies provide arguments in favour of a limitation of metabolic inflammation. This is also the case for observational studies depicting inverse association between plasma lycopene levels and inflammation. Nevertheless, current data of intervention studies are mixed concerning the anti-inflammatory effect of tomato and tomato-derived products and are not in favour of an anti-inflammatory effect of pure lycopene in humans. From epidemiological to mechanistic studies, this review aims to identify limitations of the current knowledge and gaps that remain to be filled to improve our comprehension in contrasted anti-inflammatory effects of tomato, tomato-derived products and pure lycopene.

Published
2023
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49. Post-Harvest Atmospheric Pressure and Composition Modify the Concentration and Bioaccessibility of α - and β -Carotene in Carrots and Sweet Potatoes.

Author

Hamieh B, Borel P, Raouche S, Bruzzese L, Adjriou N, Halimi C, Marconot G, Gillet G, Rostain JC, Guieu R, and Desmarchelier C

Abstract

Provitamin A (proVA) carotenoid synthesis and degradation are strongly influenced by environmental factors, including during post-harvest storage. Hypobaric and hyperbaric storages increase the shelf-life of many crops, but their effects on proVA carotenoids are not known. Our aim was to investigate the effects of modifications of atmospheric pressure and composition on α - and β -carotene concentration and bioaccessibility during the post-harvest storage of carrots and sweet potatoes. Vegetables were stored for 11-14 days at 20 °C in the dark in chambers with modified pressure and O 2 concentrations. In carrots, α - and β -carotene concentrations increased significantly during storage, but compared to the control, they were significantly lower in hyperbaria (-23 and -26%, respectively), whereas they did not differ significantly in hypoxia and hypobaria. In sweet potatoes, α - and β -carotene concentrations decreased significantly during storage, but neither hypoxia, hypobaria nor hyperbaria led to any significant change compared to the control. There was a significant increase for carrot α - and β -carotene bioaccessibility in hypobaria and hyperbaria, while there was a significant decrease for sweet potato β -carotene bioaccessibility in hypobaria/hypoxia and normobaria/hypoxia (-45% and -65% vs. control, respectively). Atmospheric pressure and composition during the post-harvest storage of carrots and sweet potatoes modified the concentration and bioaccessibility of proVA carotenoids.

Published
2023
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50. The zeaxanthin present in a tomato line rich in this carotenoid is as bioavailable as that present in the food sources richest in this xanthophyll.

Author

Morand-Laffargue L, Hirschberg J, Halimi C, Desmarchelier C, and Borel P

Subjects
Humans, Zeaxanthins, Caco-2 Cells, Xanthophylls, Carotenoids, Lutein, Solanum lycopersicum
Abstract

It is strongly suspected that, like lutein, zeaxanthin (ZEA) plays a biological role in the human eye. Many studies also suggest that it could reduce the risk of age-related macular degeneration and improve cognition. Unfortunately, it is only present in a very limited number of foods. This is why a new tomato line, named "Xantomato", whose fruits can synthesize this compound, was generated. However, whether ZEA in Xantomato is bioavailable enough for Xantomato to qualify as a nutritionally relevant ZEA source is not known. The objective was to compare the bioaccessibility and intestinal cell uptake efficiency of ZEA from Xantomato to that present in the richest sources of this compound. Bioaccessibility was assessed using in vitro digestions and uptake efficiency using Caco-2 cells. Xantomato ZEA bioaccessibility was not statistically different from that of common fruits and vegetables rich in this compound. Xantomato ZEA uptake efficiency (7.8%) was lower (P < 0.05) than that of orange pepper (10.6%) but not different from that of corn (6.9%). Therefore, the results of the in vitro digestion/Caco-2 cell model suggest that Xantomato ZEA could be as bioavailable as that found in common food sources of this compound., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published
2023
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