L-dehydroascorbic acid can substitute L-ascorbic acid as dietary vitamin C source in guinea pigs
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L-dehydroascorbic acid can substitute L-ascorbic acid as dietary vitamin C source in guinea pigs. / Frikke-Schmidt, Henriette Rønne; Tveden-Nyborg, Pernille; Lykkesfeldt, Jens.
In: Redox Biology, Vol. 7, 2016, p. 8-13.Research output: Contribution to journal › Journal article › Research › peer-review
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TY - JOUR
T1 - L-dehydroascorbic acid can substitute L-ascorbic acid as dietary vitamin C source in guinea pigs
AU - Frikke-Schmidt, Henriette Rønne
AU - Tveden-Nyborg, Pernille
AU - Lykkesfeldt, Jens
N1 - Copyright © 2015 The Authors. Published by Elsevier B.V. All rights reserved.
PY - 2016
Y1 - 2016
N2 - Vitamin C deficiency globally affects several hundred million people and has been associated with increased morbidity and mortality in numerous studies. In this study, bioavailability of the oxidized form of vitamin C (l-dehydroascorbic acid or DHA)-commonly found in vitamin C containing food products prone to oxidation-was studied. Our aim was to compare tissue accumulation of vitamin C in guinea pigs receiving different oral doses of either ascorbate or DHA. In all tissues tested (plasma, liver, spleen, lung, adrenal glands, kidney, muscle, heart, and brain), only sporadic differences in vitamin C accumulation from ascorbate or DHA were observed except for the lowest dose of DHA (0.25mg/ml in the drinking water), where approximately half of the tissues had slightly yet significantly less vitamin C accumulation than from the ascorbate source. As these results contradicted data from rats, we continued to explore the ability to recycle DHA in blood, liver and intestine in guinea pigs, rats and mice. These investigations revealed that guinea pigs have similar recycling capacity in red blood cells as observed in humans, while rats and mice do not have near the same ability to reduce DHA in erythrocytes. In liver and intestinal homogenates, guinea pigs also showed a significantly higher ability to recycle DHA compared to rats and mice. These data demonstrate that DHA in guinea pigs-as in humans-is almost as effective as ascorbate as vitamin C source when it comes to taking up and storing vitamin C and further suggest that the guinea pig is superior to other rodents in modeling human vitamin C homeostasis.
AB - Vitamin C deficiency globally affects several hundred million people and has been associated with increased morbidity and mortality in numerous studies. In this study, bioavailability of the oxidized form of vitamin C (l-dehydroascorbic acid or DHA)-commonly found in vitamin C containing food products prone to oxidation-was studied. Our aim was to compare tissue accumulation of vitamin C in guinea pigs receiving different oral doses of either ascorbate or DHA. In all tissues tested (plasma, liver, spleen, lung, adrenal glands, kidney, muscle, heart, and brain), only sporadic differences in vitamin C accumulation from ascorbate or DHA were observed except for the lowest dose of DHA (0.25mg/ml in the drinking water), where approximately half of the tissues had slightly yet significantly less vitamin C accumulation than from the ascorbate source. As these results contradicted data from rats, we continued to explore the ability to recycle DHA in blood, liver and intestine in guinea pigs, rats and mice. These investigations revealed that guinea pigs have similar recycling capacity in red blood cells as observed in humans, while rats and mice do not have near the same ability to reduce DHA in erythrocytes. In liver and intestinal homogenates, guinea pigs also showed a significantly higher ability to recycle DHA compared to rats and mice. These data demonstrate that DHA in guinea pigs-as in humans-is almost as effective as ascorbate as vitamin C source when it comes to taking up and storing vitamin C and further suggest that the guinea pig is superior to other rodents in modeling human vitamin C homeostasis.
KW - Faculty of Health and Medical Sciences
KW - Vitamin C
KW - Bioavailability
KW - Ascorbate recycling
KW - Guinea pig
KW - Rat
KW - Mouse
KW - Human
U2 - 10.1016/j.redox.2015.11.003
DO - 10.1016/j.redox.2015.11.003
M3 - Journal article
C2 - 26609560
VL - 7
SP - 8
EP - 13
JO - Redox Biology
JF - Redox Biology
SN - 2213-2317
ER -
ID: 152241591