Low β-carotene bioaccessibility and bioavailability from high fat, dairy-based meal

dc.contributor.authorKruger, Johanita
dc.contributor.authorSus, Nadine
dc.contributor.authorMoser, Andrea
dc.contributor.authorScholz, Sophie
dc.contributor.authorAdler, Guenther
dc.contributor.authorVenturelli, Sascha
dc.contributor.authorFrank, Jan
dc.date.accessioned2024-10-22T09:45:19Z
dc.date.available2024-10-22T09:45:19Z
dc.date.issued2024-09
dc.description.abstractPURPOSE : The original aim of the study was to determine, in a double-blind 3-arm crossover human trial (n = 7), the effect of supplemental levels of iron (25 mg) and zinc (30 mg) on β-carotene (synthetic) bioavailability (10 h postprandial). However, despite the high dose of supplemental β-carotene (15 mg) consumed with the high fat (18 g), dairy-based breakfast test meal, there was a negligible postprandial response in plasma and triglyceride rich fraction β-carotene concentrations. We then systematically investigated the possible reasons for this low bioavailability of β-carotene. METHODS : We determined (1) if the supplemental β-carotene could be micellised and absorbed by epithelial cells, using a Caco-2 cell model, (2) if the fat from the test meal was sufficiently bioavailable to facilitate β-carotene bioavailability, (3) the extent to which the β-carotene could have been metabolised and converted to retinoic acid/retinol and (4) the effect of the test meal matrix on the β-carotene bioaccessibility (in vitro digestion) and Caco-2 cellular uptake. RESULTS : We found that (1) The supplemental β-carotene could be micellised and absorbed by epithelial cells, (2) the postprandial plasma triacylglycerol response was substantial (approximately 75–100 mg dL−1 over 10 h), indicating sufficient lipid bioavailability to ensure β-carotene absorption, (3) the high fat content of the meal (approximately 18 g) could have resulted in increased β-carotene metabolism, (4) β-carotene bioaccessibility from the dairy-based test meal was sixfold lower (p < 0.05) than when digested with olive oil. CONCLUSION : The low β-carotene bioavailability is probably due to a combination of the metabolism of β-carotene to retinol by BCMO1 and interactions of β-carotene with the food matrix, decreasing the bioaccessibility. TRAIL REGISTRATION : The human trail was retrospectively registered (ClinicalTrail.gov ID: NCT05840848).en_US
dc.description.departmentConsumer Scienceen_US
dc.description.departmentFood Scienceen_US
dc.description.librarianhj2024en_US
dc.description.sdgSDG-02:Zero Hungeren_US
dc.description.sponsorshipA Georg Forster Research Fellowship from the Alexander von Humboldt Foundation. Open Access funding enabled and organized by Projekt DEAL.en_US
dc.description.urihttp://link.springer.com/journal/394en_US
dc.identifier.citationKruger, J., Sus, N., Moser, A. et al. Low β-carotene bioaccessibility and bioavailability from high fat, dairy-based meal. European Journal of Nutrition 63, 2261–2270 (2024). https://doi.org/10.1007/s00394-024-03423-w.en_US
dc.identifier.issn1436-6207 (print)
dc.identifier.issn1436-6215 (online)
dc.identifier.other10.1007/s00394-024-03423-w
dc.identifier.urihttp://hdl.handle.net/2263/98704
dc.language.isoenen_US
dc.publisherSpringeren_US
dc.rights© The Author(s) 2024. Open Access. This article is licensed under a Creative Commons Attribution 4.0 International License.en_US
dc.subjectBioaccessibilityen_US
dc.subjectCellular uptakeen_US
dc.subjectDivalent mineralsen_US
dc.subjectFood matrixen_US
dc.subjectLipid profileen_US
dc.subjectMicellizationen_US
dc.subjectDairyen_US
dc.subjectBCMO1en_US
dc.subjectSDG-02: Zero hungeren_US
dc.titleLow β-carotene bioaccessibility and bioavailability from high fat, dairy-based mealen_US
dc.typeArticleen_US

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