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大鼠小肠中两种维生素A代谢酶和两种视黄醇结合蛋白的个体发生。

Ontogeny of two vitamin A-metabolizing enzymes and two retinol-binding proteins present in the small intestine of the rat.

作者信息

Ong D E, Lucas P C, Kakkad B, Quick T C

机构信息

Department of Biochemistry, Vanderbilt University School of Medicine, Nashville, TN 37232.

出版信息

J Lipid Res. 1991 Sep;32(9):1521-7.

PMID:1753219
Abstract

The patterns of expression of cellular retinol-binding protein (CRBP), cellular retinol-binding protein, type two [CRBP(II)], lecithin: retinol acyltransferase (LRAT), and microsomal retinal reductase were examined for rat small intestine during the perinatal period. CRBP was present (15 pmole per mg soluble protein) at the earliest time examined, the 16th day of gestation, declining by 70% by birth, maintained to adulthood. In contrast, CRBP(II) appeared 2-3 days before birth, rising to its highest level (500 pmole per mg soluble protein) by day 3 after birth, then declining by 50% during the late suckling period to the adult level. Immunohistochemistry revealed that CRBP(II) initially appeared in the epithelial cell layer in a patchy manner, resolving by birth into an even staining of all villus-associated enterocytes. In contrast, CRBP was evenly expressed in the epithelial cell layer at day 17/18 but was absent by birth. Intestinal LRAT activity increased rapidly in the 2 days prior to birth, then declined at weaning to the adult level. Microsomal retinal reductase was measurable in the intestine at birth, but not detected during the early suckling period, reappearing at day 21. Considerable increase was then observed coincident with weaning, when carotenes, from which retinal is derived, became an important source of vitamin A. The pattern of appearance of these elements appears to prepare the intestine for the necessary processing of vitamin A required after birth.

摘要

在围产期对大鼠小肠中细胞视黄醇结合蛋白(CRBP)、细胞视黄醇结合蛋白2型[CRBP(II)]、卵磷脂:视黄醇酰基转移酶(LRAT)和微粒体视黄醛还原酶的表达模式进行了研究。最早在妊娠第16天检测时就存在CRBP(每毫克可溶性蛋白15皮摩尔),到出生时下降70%,并维持到成年期。相比之下,CRBP(II)在出生前2 - 3天出现,出生后第3天升至最高水平(每毫克可溶性蛋白500皮摩尔),然后在哺乳后期下降50%至成年水平。免疫组织化学显示,CRBP(II)最初以斑片状出现在上皮细胞层,出生时逐渐变为所有绒毛相关肠细胞的均匀染色。相反,CRBP在第17/18天在上皮细胞层均匀表达,但出生时不存在。肠道LRAT活性在出生前2天迅速增加,然后在断奶时下降至成年水平。微粒体视黄醛还原酶在出生时可在肠道中检测到,但在哺乳早期未检测到,在第21天重新出现。然后观察到在断奶时,与视黄醛来源的胡萝卜素成为维生素A的重要来源同时,该酶有相当大的增加。这些成分的出现模式似乎为出生后肠道对维生素A所需的必要加工做准备。

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