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α-视黄醇通过泌乳母猪-哺乳仔猪对的血清视黄醇结合蛋白非依赖性机制进行分布。

α-Retinol is distributed through serum retinol-binding protein-independent mechanisms in the lactating sow-nursing piglet dyad.

机构信息

Nutritional Sciences Department, University of Wisconsin, Madison, WI 53706, USA.

出版信息

J Nutr. 2011 Jan;141(1):42-7. doi: 10.3945/jn.110.127597. Epub 2010 Nov 10.

Abstract

α-Retinol (αR) is a structural isomer of retinol [vitamin A (VA)] that does not bind to serum retinol-binding protein (RBP). In this study, α-retinyl acetate (αRA) was synthesized and given orally (35 μmol) to VA-deficient lactating sows (n = 11) to assess its potential to trace RBP-independent retinol transport and tissue uptake. The αRA dose primarily appeared in sow serum as 4 α-retinyl esters (αRE) with peak serum total αR concentrations (the sum of the alcohol and ester forms) detected at 2 h (70 ± 23 nmol/L, mean ± SEM) postdose. From 0 to 40 h postdose, the percentage of serum total αR in the alcohol form did not increase. Rapid αR uptake into sow milk was observed with peak concentrations (371 ± 83 nmol/L) at 7.5 h postdose, consistent with the uptake of αRE from chylomicra. A high percentage of the αRA dose (62 ± 15%, mean ± SD) was present in the livers of sows (n = 6) killed 22-28 d postdose. Approximately 15-26% of the sow αRA dose was transferred to the livers of the nursing piglets (n = 17) after 3 d. In piglets and sows, a similar percentage of hepatic total αR was detected in the ester form as that of hepatic total retinol. Taken together, these data suggest that an oral dose of αRA effectively traces the uptake, esterification, chylomicron transport, and hepatic storage of retinol and may be useful for deciphering the role of RBP-independent delivery of retinol to other tissues.

摘要

α-视黄醇(αR)是视黄醇[维生素 A(VA)]的结构异构体,不与血清视黄醇结合蛋白(RBP)结合。在这项研究中,α-视黄基乙酸酯(αRA)被合成并口服给予 VA 缺乏的哺乳期母猪(n = 11),以评估其追踪不依赖 RBP 的视黄醇转运和组织摄取的潜力。αRA 剂量主要以 4 种 α-视黄基酯(αRE)的形式出现在母猪血清中,给药后 2 小时(70 ± 23 nmol/L,均值 ± SEM)检测到血清总 αR 浓度峰值。在 0 到 40 小时期间,血清总 αR 以醇形式存在的比例没有增加。观察到母猪乳汁中 αR 的摄取速度很快,给药后 7.5 小时达到峰值浓度(371 ± 83 nmol/L),与乳糜微粒中 αRE 的摄取一致。给予的 αRA 剂量(62 ± 15%,均值 ± SD)的很大一部分(n = 6)存在于 22-28 天处死的母猪肝脏中。在 3 天后,母猪的 αRA 剂量的约 15-26%转移到哺乳仔猪(n = 17)的肝脏中。在仔猪和母猪中,肝总 αR 的酯形式百分比与肝总视黄醇相似。综合这些数据表明,口服给予 αRA 可以有效地追踪视黄醇的摄取、酯化、乳糜微粒转运和肝脏储存,并且可能有助于解析视黄醇不依赖 RBP 向其他组织输送的作用。

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