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胆红素还原酶的多种形式:大鼠肝脏和大脑中表达模式的年龄相关变化。

Multiple forms of biliverdin reductase: age-related change in pattern of expression in rat liver and brain.

作者信息

Maines M D

机构信息

University of Rochester School of Medicine, Department of Biophysics, New York 14642.

出版信息

Mol Pharmacol. 1990 Oct;38(4):481-5.

PMID:2233689
Abstract

Biliverdin reductase is the dual nucleotide-dependent cytosolic enzyme that converts biliverdin to the bile pigment, bilirubin, and displays extensive microheterogeneity in rat organs. The enzyme is unique in having two pH optima. The present study reports on the tissue-dependent pattern of developmental expression of the reductase in rat liver and brain. When analyzed by Western immunoblotting, two closely migrating immunoreactive proteins were detected in the liver cytosol during the first 2-3 weeks after birth; the protein with greater mobility was not detected in the liver of adult aged animals (6 months old) and was present at low levels in rats during the first week of life. The faster migrating protein was not detected in the brain cytosol at any stage of development. Furthermore, in the brain the total amount of enzyme protein increased as the animal matured, whereas in the liver the enzyme protein level decreased with age. When the purified enzyme was analyzed, age-related changes in the variant composition of the enzyme in the liver were noted. Although in both adult and newborn animals (14 days old) the purified enzyme, when subjected to isoelectric focusing, separates into five net charge forms (pl 6.23, 5.91, 5.76, 5.61, and 5.48), the relative abundance of the variants notably differed in the two preparations. In addition, when the purified preparations were subjected to two-dimensional electrophoresis, although both purified preparations separate into three molecular weight forms (Mr 30,400, 30,700, and 31,400) one species (Mr 31,400, pl = 5.77), which was very prominently expressed in the newborn, was essentially absent in the adult. Biliverdin reductase activity of the liver cytosol with both NADPH (pH 8.7) and NADH (pH 6.7) exhibited developmental changes, with the activity increasing after birth, reaching a peak on day 14, and decreasing to low levels in the adult. The existence of a close correlation between development of biliverdin reductase activity in the brain and liver and that of heme oxygenase in these organs is noted. The suggestion is made that the reductase is not a passive component of the heme degradation pathway; rather, its activity could become limiting in the elimination of heme degradation products.

摘要

胆绿素还原酶是一种依赖双核苷酸的胞质酶,可将胆绿素转化为胆汁色素胆红素,并且在大鼠器官中表现出广泛的微异质性。该酶具有两个最适pH值,这一点很独特。本研究报道了大鼠肝脏和大脑中还原酶发育表达的组织依赖性模式。通过蛋白质免疫印迹分析发现,出生后的前2 - 3周,在肝脏胞质溶胶中检测到两种迁移距离相近的免疫反应性蛋白;迁移速度较快的那种蛋白在成年动物(6个月大)的肝脏中未检测到,而在出生后第一周的大鼠体内含量较低。在发育的任何阶段,迁移速度较快的那种蛋白在大脑胞质溶胶中均未检测到。此外,在大脑中,酶蛋白的总量随着动物的成熟而增加,而在肝脏中,酶蛋白水平随年龄增长而下降。对纯化后的酶进行分析时,发现肝脏中酶变体组成存在与年龄相关的变化。尽管在成年动物和新生动物(14日龄)中,纯化后的酶在进行等电聚焦时均分离为五种净电荷形式(等电点分别为6.23、5.91、5.76、5.61和5.48),但两种制剂中这些变体的相对丰度明显不同。此外,当对纯化制剂进行二维电泳时,尽管两种纯化制剂均分离为三种分子量形式(分子量分别为30,400、30,700和31,400),但有一种在新生动物中非常显著表达的形式(分子量为31,400,等电点 = 5.77)在成年动物中基本不存在。肝脏胞质溶胶中以NADPH(pH 8.7)和NADH(pH 6.7)为底物时的胆绿素还原酶活性呈现出发育变化,出生后活性增加,在第14天达到峰值,然后在成年时降至低水平。研究发现大脑和肝脏中胆绿素还原酶活性的发育与这些器官中血红素加氧酶的发育之间存在密切相关性。有人提出,还原酶并非血红素降解途径中的被动成分;相反,其活性在血红素降解产物的清除过程中可能成为限制因素。

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