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Host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans

Carotenoid dietary intake and their endogenous levels have been associated with a decreased risk of several chronic diseases. There are indications that carotenoid bioavailability depends, in addition to the food matrix, on host factors. These include diseases (e.g. colitis), life‐style habits (e.g....

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Autores principales: Bohn, Torsten, Desmarchelier, Charles, Dragsted, Lars O., Nielsen, Charlotte S., Stahl, Wilhelm, Rühl, Ralph, Keijer, Jaap, Borel, Patrick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5516247/
https://www.ncbi.nlm.nih.gov/pubmed/28101967
http://dx.doi.org/10.1002/mnfr.201600685
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author Bohn, Torsten
Desmarchelier, Charles
Dragsted, Lars O.
Nielsen, Charlotte S.
Stahl, Wilhelm
Rühl, Ralph
Keijer, Jaap
Borel, Patrick
author_facet Bohn, Torsten
Desmarchelier, Charles
Dragsted, Lars O.
Nielsen, Charlotte S.
Stahl, Wilhelm
Rühl, Ralph
Keijer, Jaap
Borel, Patrick
author_sort Bohn, Torsten
collection PubMed
description Carotenoid dietary intake and their endogenous levels have been associated with a decreased risk of several chronic diseases. There are indications that carotenoid bioavailability depends, in addition to the food matrix, on host factors. These include diseases (e.g. colitis), life‐style habits (e.g. smoking), gender and age, as well as genetic variations including single nucleotide polymorphisms that govern carotenoid metabolism. These are expected to explain interindividual differences that contribute to carotenoid uptake, distribution, metabolism and excretion, and therefore possibly also their association with disease risk. For instance, digestion enzymes fostering micellization (PNLIP, CES), expression of uptake/efflux transporters (SR‐BI, CD36, NPC1L1), cleavage enzymes (BCO1/2), intracellular transporters (FABP2), secretion into chylomicrons (APOB, MTTP), carotenoid metabolism in the blood and liver (LPL, APO C/E, LDLR), and distribution to target tissues such as adipose tissue or macula (GSTP1, StARD3) depend on the activity of these proteins. In addition, human microbiota, e.g. via altering bile‐acid concentrations, may play a role in carotenoid bioavailability. In order to comprehend individual, variable responses to these compounds, an improved knowledge on intra‐/interindividual factors determining carotenoid bioavailability, including tissue distribution, is required. Here, we highlight the current knowledge on factors that may explain such intra‐/interindividual differences.
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spelling pubmed-55162472017-08-02 Host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans Bohn, Torsten Desmarchelier, Charles Dragsted, Lars O. Nielsen, Charlotte S. Stahl, Wilhelm Rühl, Ralph Keijer, Jaap Borel, Patrick Mol Nutr Food Res Reviews Carotenoid dietary intake and their endogenous levels have been associated with a decreased risk of several chronic diseases. There are indications that carotenoid bioavailability depends, in addition to the food matrix, on host factors. These include diseases (e.g. colitis), life‐style habits (e.g. smoking), gender and age, as well as genetic variations including single nucleotide polymorphisms that govern carotenoid metabolism. These are expected to explain interindividual differences that contribute to carotenoid uptake, distribution, metabolism and excretion, and therefore possibly also their association with disease risk. For instance, digestion enzymes fostering micellization (PNLIP, CES), expression of uptake/efflux transporters (SR‐BI, CD36, NPC1L1), cleavage enzymes (BCO1/2), intracellular transporters (FABP2), secretion into chylomicrons (APOB, MTTP), carotenoid metabolism in the blood and liver (LPL, APO C/E, LDLR), and distribution to target tissues such as adipose tissue or macula (GSTP1, StARD3) depend on the activity of these proteins. In addition, human microbiota, e.g. via altering bile‐acid concentrations, may play a role in carotenoid bioavailability. In order to comprehend individual, variable responses to these compounds, an improved knowledge on intra‐/interindividual factors determining carotenoid bioavailability, including tissue distribution, is required. Here, we highlight the current knowledge on factors that may explain such intra‐/interindividual differences. John Wiley and Sons Inc. 2017-02-27 2017-06 /pmc/articles/PMC5516247/ /pubmed/28101967 http://dx.doi.org/10.1002/mnfr.201600685 Text en © 2017 The Authors. Molecular Nutrition & Food Research published by WILEY‐VCH Verlag GmbH & Co. KGaA, Weinheim This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Reviews
Bohn, Torsten
Desmarchelier, Charles
Dragsted, Lars O.
Nielsen, Charlotte S.
Stahl, Wilhelm
Rühl, Ralph
Keijer, Jaap
Borel, Patrick
Host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans
title Host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans
title_full Host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans
title_fullStr Host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans
title_full_unstemmed Host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans
title_short Host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans
title_sort host‐related factors explaining interindividual variability of carotenoid bioavailability and tissue concentrations in humans
topic Reviews
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5516247/
https://www.ncbi.nlm.nih.gov/pubmed/28101967
http://dx.doi.org/10.1002/mnfr.201600685
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