Vitamin A supplementation increases the uptake of chylomicron retinyl esters into the brain of neonatal rats raised under vitamin A-marginal conditions

Joanna K. Hodges; Libo Tan; Michael H. Green; A. Catharine Ross

doi:10.3945/jn.116.233692

Vitamin A supplementation increases the uptake of chylomicron retinyl esters into the brain of neonatal rats raised under vitamin A-marginal conditions

Joanna K. Hodges, Libo Tan, Michael H. Green, A. Catharine Ross

Nutritional Sciences

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Background: The most rapid phase of brain development occurs during the neonatal period. Vitamin A (VA; retinol) iscritical for many aspects of this process, including neurogenesis, synaptic plasticity, learning, and memory formation.However, the metabolism of retinol in the neonatal brain has not been extensively explored.Objective: We examined the uptake of VA into the brain in neonatal rats raised under VA-marginal conditions (controlgroup) and assessed the effect of VA supplementation on the uptake of VA into the brain.Methods: Sprague-Dawley neonatal rats (n = 104) nursed by mothers fed a VA-marginal diet were randomly assigned andtreated on postnatal day 4 with an oral dose of either VA (6 mg retinyl palmitate/g body weight) or canola oil as the control,both of which contained 1.8 μCi [³H]retinol. Pups (n = 4/group at a time) were killed at 13 sampling times from 30 min to24 d after dosing. The uptake of total retinol, chylomicron-associated retinyl esters (REs), and retinol bound to retinolbindingprotein (RBP) was estimated with the use of WinSAAM version 3.0.8.Results: Total retinol mass in the brain was closely dependent on its mass in plasma over time (r = 0.91; P < 0.001). Theuptake of retinol into the brain involved both postprandial chylomicrons and RBP, with RBP delivering most of the retinol inthe control group [0.27 nmol/d (RBP) compared with 0.01 nmol/d (chylomicrons)]. VA supplementation increased thefractional uptake of chylomicron REs from 0.3% to 1.2% of plasma pool/d, decreased that of RBP retinol from 0.5% to0.2% of plasma pool/d, and increased the transfer rate of chylomicron REs from nearly zero to 0.7 nmol/d, causing a daylongelevation in the brain mass of total retinol.Conclusion: Postprandial chylomicrons may be a primary mechanism for delivering a recently ingested large dose of VA tothe brain of neonatal rats raised under VA-marginal conditions.

Original language	English (US)
Pages (from-to)	1677-1683
Number of pages	7
Journal	Journal of Nutrition
Volume	146
Issue number	9
DOIs	https://doi.org/10.3945/jn.116.233692
State	Published - 2016

All Science Journal Classification (ASJC) codes

Medicine (miscellaneous)
Nutrition and Dietetics

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@article{0f0d24f10ee04e31b5b5598e775dab77,

title = "Vitamin A supplementation increases the uptake of chylomicron retinyl esters into the brain of neonatal rats raised under vitamin A-marginal conditions",

abstract = "Background: The most rapid phase of brain development occurs during the neonatal period. Vitamin A (VA; retinol) iscritical for many aspects of this process, including neurogenesis, synaptic plasticity, learning, and memory formation.However, the metabolism of retinol in the neonatal brain has not been extensively explored.Objective: We examined the uptake of VA into the brain in neonatal rats raised under VA-marginal conditions (controlgroup) and assessed the effect of VA supplementation on the uptake of VA into the brain.Methods: Sprague-Dawley neonatal rats (n = 104) nursed by mothers fed a VA-marginal diet were randomly assigned andtreated on postnatal day 4 with an oral dose of either VA (6 mg retinyl palmitate/g body weight) or canola oil as the control,both of which contained 1.8 μCi [3H]retinol. Pups (n = 4/group at a time) were killed at 13 sampling times from 30 min to24 d after dosing. The uptake of total retinol, chylomicron-associated retinyl esters (REs), and retinol bound to retinolbindingprotein (RBP) was estimated with the use of WinSAAM version 3.0.8.Results: Total retinol mass in the brain was closely dependent on its mass in plasma over time (r = 0.91; P < 0.001). Theuptake of retinol into the brain involved both postprandial chylomicrons and RBP, with RBP delivering most of the retinol inthe control group [0.27 nmol/d (RBP) compared with 0.01 nmol/d (chylomicrons)]. VA supplementation increased thefractional uptake of chylomicron REs from 0.3% to 1.2% of plasma pool/d, decreased that of RBP retinol from 0.5% to0.2% of plasma pool/d, and increased the transfer rate of chylomicron REs from nearly zero to 0.7 nmol/d, causing a daylongelevation in the brain mass of total retinol.Conclusion: Postprandial chylomicrons may be a primary mechanism for delivering a recently ingested large dose of VA tothe brain of neonatal rats raised under VA-marginal conditions.",

author = "Hodges, {Joanna K.} and Libo Tan and Green, {Michael H.} and Ross, {A. Catharine}",

note = "Publisher Copyright: {\textcopyright} 2016 American Society for Nutrition.",

year = "2016",

doi = "10.3945/jn.116.233692",

language = "English (US)",

volume = "146",

pages = "1677--1683",

journal = "Journal of Nutrition",

issn = "0022-3166",

publisher = "Elsevier B.V.",

number = "9",

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TY - JOUR

T1 - Vitamin A supplementation increases the uptake of chylomicron retinyl esters into the brain of neonatal rats raised under vitamin A-marginal conditions

AU - Hodges, Joanna K.

AU - Tan, Libo

AU - Green, Michael H.

AU - Ross, A. Catharine

PY - 2016

Y1 - 2016

N2 - Background: The most rapid phase of brain development occurs during the neonatal period. Vitamin A (VA; retinol) iscritical for many aspects of this process, including neurogenesis, synaptic plasticity, learning, and memory formation.However, the metabolism of retinol in the neonatal brain has not been extensively explored.Objective: We examined the uptake of VA into the brain in neonatal rats raised under VA-marginal conditions (controlgroup) and assessed the effect of VA supplementation on the uptake of VA into the brain.Methods: Sprague-Dawley neonatal rats (n = 104) nursed by mothers fed a VA-marginal diet were randomly assigned andtreated on postnatal day 4 with an oral dose of either VA (6 mg retinyl palmitate/g body weight) or canola oil as the control,both of which contained 1.8 μCi [3H]retinol. Pups (n = 4/group at a time) were killed at 13 sampling times from 30 min to24 d after dosing. The uptake of total retinol, chylomicron-associated retinyl esters (REs), and retinol bound to retinolbindingprotein (RBP) was estimated with the use of WinSAAM version 3.0.8.Results: Total retinol mass in the brain was closely dependent on its mass in plasma over time (r = 0.91; P < 0.001). Theuptake of retinol into the brain involved both postprandial chylomicrons and RBP, with RBP delivering most of the retinol inthe control group [0.27 nmol/d (RBP) compared with 0.01 nmol/d (chylomicrons)]. VA supplementation increased thefractional uptake of chylomicron REs from 0.3% to 1.2% of plasma pool/d, decreased that of RBP retinol from 0.5% to0.2% of plasma pool/d, and increased the transfer rate of chylomicron REs from nearly zero to 0.7 nmol/d, causing a daylongelevation in the brain mass of total retinol.Conclusion: Postprandial chylomicrons may be a primary mechanism for delivering a recently ingested large dose of VA tothe brain of neonatal rats raised under VA-marginal conditions.

AB - Background: The most rapid phase of brain development occurs during the neonatal period. Vitamin A (VA; retinol) iscritical for many aspects of this process, including neurogenesis, synaptic plasticity, learning, and memory formation.However, the metabolism of retinol in the neonatal brain has not been extensively explored.Objective: We examined the uptake of VA into the brain in neonatal rats raised under VA-marginal conditions (controlgroup) and assessed the effect of VA supplementation on the uptake of VA into the brain.Methods: Sprague-Dawley neonatal rats (n = 104) nursed by mothers fed a VA-marginal diet were randomly assigned andtreated on postnatal day 4 with an oral dose of either VA (6 mg retinyl palmitate/g body weight) or canola oil as the control,both of which contained 1.8 μCi [3H]retinol. Pups (n = 4/group at a time) were killed at 13 sampling times from 30 min to24 d after dosing. The uptake of total retinol, chylomicron-associated retinyl esters (REs), and retinol bound to retinolbindingprotein (RBP) was estimated with the use of WinSAAM version 3.0.8.Results: Total retinol mass in the brain was closely dependent on its mass in plasma over time (r = 0.91; P < 0.001). Theuptake of retinol into the brain involved both postprandial chylomicrons and RBP, with RBP delivering most of the retinol inthe control group [0.27 nmol/d (RBP) compared with 0.01 nmol/d (chylomicrons)]. VA supplementation increased thefractional uptake of chylomicron REs from 0.3% to 1.2% of plasma pool/d, decreased that of RBP retinol from 0.5% to0.2% of plasma pool/d, and increased the transfer rate of chylomicron REs from nearly zero to 0.7 nmol/d, causing a daylongelevation in the brain mass of total retinol.Conclusion: Postprandial chylomicrons may be a primary mechanism for delivering a recently ingested large dose of VA tothe brain of neonatal rats raised under VA-marginal conditions.

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Vitamin A supplementation increases the uptake of chylomicron retinyl esters into the brain of neonatal rats raised under vitamin A-marginal conditions

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