大鼠乳腺中的锌转运体在哺乳期对边缘性锌和维生素A摄入量作出反应。
Zinc transporters in the rat mammary gland respond to marginal zinc and vitamin A intakes during lactation.
作者信息
Kelleher Shannon L, Lönnerdal Bo
机构信息
Department of Nutrition, University of California, Davis, CA 95616, USA.
出版信息
J Nutr. 2002 Nov;132(11):3280-5. doi: 10.1093/jn/132.11.3280.
Marginal intake of zinc and vitamin A is common during lactation and a deficiency of one micronutrient can result in a secondary deficiency of the other. However, the resistance of milk zinc (Zn) concentration to changes in dietary Zn or vitamin A indicates tight regulation of mammary gland Zn transport. Although several mammalian proteins have been identified and implicated in Zn transport, the mechanisms responsible for mammary gland Zn transport and their regulation by dietary Zn and vitamin A are unknown. In this study, we identified mammary gland Zn transporters and determined effects of marginal Zn and vitamin A intakes on their levels. Rats were fed a control [25 mg Zn/kg, 4 retinol equivalents (RE)/g], a low Zn (10 mg Zn/kg), a low vitamin A (0.4 RE/g), or a low Zn (10 mg Zn/kg) and vitamin A (0.4 RE/g) diet throughout lactation. ZnT-1, ZnT-2 and ZnT-4 were identified in the mammary gland and localized to the serosal membrane (ZnT-1) or intracellularly (ZnT-2 and ZnT-4) by immunostaining. Rats fed a low Zn or low vitamin A diet had lower ZnT-1 protein and higher ZnT-4 mRNA expression and protein levels compared with controls. There was a significant interaction between dietary Zn and vitamin A on zinc transporter mRNA expression and protein levels. Although total mammary gland Zn was not affected, mammary gland metallothionein levels were lower in rats fed low Zn and higher in rats fed low vitamin A, suggesting different mechanisms regulating zinc transporter levels. These results indicate that milk Zn level is maintained through coordinated regulation of mammary gland zinc transporters and documents an effect of vitamin A on zinc homeostasis at the molecular level during lactation.
哺乳期锌和维生素A的边缘性摄入很常见,一种微量营养素缺乏会导致另一种微量营养素的继发性缺乏。然而,乳锌(Zn)浓度对膳食锌或维生素A变化的抗性表明乳腺锌转运受到严格调控。尽管已经鉴定出几种与锌转运有关的哺乳动物蛋白,但负责乳腺锌转运的机制及其受膳食锌和维生素A调控的机制尚不清楚。在本研究中,我们鉴定了乳腺锌转运体,并确定了边缘性锌和维生素A摄入对其水平的影响。在整个哺乳期,给大鼠喂食对照饮食[25 mg锌/千克,4视黄醇当量(RE)/克]、低锌饮食(10 mg锌/千克)、低维生素A饮食(0.4 RE/克)或低锌(10 mg锌/千克)和维生素A(0.4 RE/克)饮食。通过免疫染色在乳腺中鉴定出锌转运体1(ZnT-1)、锌转运体2(ZnT-2)和锌转运体4(ZnT-4),并将其定位到浆膜(ZnT-1)或细胞内(ZnT-2和ZnT-4)。与对照组相比,喂食低锌或低维生素A饮食的大鼠ZnT-1蛋白水平较低,ZnT-4 mRNA表达和蛋白水平较高。膳食锌和维生素A对锌转运体mRNA表达和蛋白水平有显著的相互作用。尽管乳腺总锌含量未受影响,但喂食低锌的大鼠乳腺金属硫蛋白水平较低,喂食低维生素A的大鼠乳腺金属硫蛋白水平较高,这表明调节锌转运体水平的机制不同。这些结果表明,乳锌水平通过乳腺锌转运体的协调调节得以维持,并证明了维生素A在哺乳期分子水平上对锌稳态的影响。
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