首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Lecithin:Retinol Acyltransferase Is Critical for Cellular Uptake of Vitamin A from Serum Retinol-binding Protein
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Lecithin:Retinol Acyltransferase Is Critical for Cellular Uptake of Vitamin A from Serum Retinol-binding Protein

机译:卵磷脂:视黄醇酰基转移酶对于从血清视黄醇结合蛋白摄取维生素A至关重要

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摘要

Vitamin A (all-trans-retinol) must be adequately distributed within the mammalian body to produce visual chromophore in the eyes and all-trans-retinoic acid in other tissues. Vitamin A is transported in the blood bound to retinol-binding protein (holo-RBP), and its target cells express an RBP receptor encoded by the Stra6 (stimulated by retinoic acid 6) gene. Here we show in mice that cellular uptake of vitamin A from holo-RBP depends on functional coupling of STRA6 with intracellular lecithin:retinol acyltransferase (LRAT). Thus, vitamin A uptake from recombinant holo-RBP exhibited by wild type mice was impaired in Lrat−/− mice. We further provide evidence that vitamin A uptake is regulated by all-trans-retinoic acid in non-ocular tissues of mice. When in excess, vitamin A was rapidly taken up and converted to its inert ester form in peripheral tissues, such as lung, whereas in vitamin A deficiency, ocular retinoid uptake was favored. Finally, we show that the drug fenretinide, used clinically to presumably lower blood RBP levels and thus decrease circulating retinol, targets the functional coupling of STRA6 and LRAT to increase cellular vitamin A uptake in peripheral tissues. These studies provide mechanistic insights into how vitamin A is distributed to peripheral tissues in a regulated manner and identify LRAT as a critical component of this process.
机译:维生素A(全反式维甲酸)必须在哺乳动物体内充分分布,以在眼睛中产生视觉发色团,并在其他组织中产生全反式维甲酸。维生素A在血液中与视黄醇结合蛋白(holo-RBP)结合运输,其靶细胞表达由Stra6(受视黄酸6刺激)基因编码的RBP受体。在这里,我们在小鼠中显示从全息RBP摄取维生素A取决于STRA6与细胞内卵磷脂:视黄醇酰基转移酶(LRAT)的功能偶联。因此,在Lrat -/-小鼠中,野生型小鼠表现出的从重组的完整RBP吸收维生素A受到损害。我们进一步提供证据表明,小鼠非眼组织中的全反式维甲酸可调节维生素A的摄取。过量时,维生素A会迅速吸收并在周围组织(如肺)中转化为惰性酯形式,而维生素A缺乏时,则有利于眼类维生素A的摄取。最后,我们表明,临床上用于降低血液RBP水平从而降低循环视黄醇的药物芬维A胺靶向STRA6和LRAT的功能偶联,以增加外周组织中细胞对维生素A的摄取。这些研究提供了有关维生素A如何以受控方式分布到周围组织的机制的见解,并确定了LRAT是该过程的关键组成部分。

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