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肠道和肾脏中存在的1,25-二羟基维生素D3新的C-23氧化代谢途径的鉴定。

Identification of a new C-23 oxidation pathway of metabolism for 1,25-dihydroxyvitamin D3 present in intestine and kidney.

作者信息

Ohnuma N, Norman A W

出版信息

J Biol Chem. 1982 Jul 25;257(14):8261-71.

PMID:6896331
Abstract

Evidence is presented for the existence of a new C-23 oxidation pathway for the metabolism of the hormonally active form of vitamin D3, namely 1 alpha,25-dihydroxyvitamin D3 (1,25(OH)2D3). Homogenates of intestinal mucosa or kidney, but not liver, from rats and chicks convert 1,25(OH)2[26,27-3H]D3 into two new metabolites, 1 alpha,25-dihydroxy-23-oxo-vitamin D3 (1,25(OH)2-23-oxo-D3) and 1 alpha,25,26-trihydroxy-23-oxo-vitamin D3 (1,25,26(OH)3-23-oxo-D3), and an unknown metabolite(s) which has been possibly subjected to side chain modification/cleavage so that the tritium of the substrate has been converted into a form which is volatile. The isolation and chemical characterization of 1,25(OH)2-23-oxo-D3 and 1,25,26(OH)3-23-oxo-D3 from homogenates of chick intestinal mucosa has recently been described (Ohnuma, N., Kruse, J., Popjak, G., and Norman, A. W. (1982) J. Biol. Chem. 257, 5097-5102). Based on kinetic studies with chick intestinal homogenates, the proposed C-23 oxidation pathway is: 1,25(OH)2D3 leads to 1,25(OH)2-23-oxo-D3 leads to 1,25,26(OH)3-23-oxo-D3 leads to unknown metabolite with altered side chain. The relative enzyme activities of the C-23 pathway in tissues from vitamin D-replete chicks are: intestine, kidney liver, 18:3:less than 1. The activity of the C-23 pathway in homogenates of chick intestinal mucosa can be enhanced 10 x by prior priming of the birds with a single intravenous dose of 500 ng (1.3 nmol) of 1,25(OH)2D3; the induction of the enzyme activity is maximal by 3-6 h and returns to basal levels by 12 h. A comparison was made in chick and rat intestinal homogenates of this C-23 pathway and the previously known C-24 oxidation pathway, which converts 1,25(OH)2D3 into 1,24,25-trihydroxyvitamin D3 (1,24,25(OH)3D3); it was calculated that under these conditions 72% of the 1,25(OH)2D3 was metabolized by the C-23 oxidation pathway, 13% by the C-24 pathway, and only 14% by other as yet unspecified pathways. It is proposed that the newly discovered C-23 pathway for metabolism of 1,25(OH)2D3 by the target intestinal mucosa and kidney may play a prominent role under physiological conditions of controlling the tissue levels of this hormonally active form of vitamin D3.

摘要

有证据表明,存在一种新的C-23氧化途径,用于激素活性形式的维生素D3,即1α,25-二羟基维生素D3(1,25(OH)2D3)的代谢。大鼠和雏鸡的肠黏膜或肾脏匀浆(而非肝脏匀浆)可将1,25(OH)2[26,27-3H]D3转化为两种新的代谢产物,即1α,25-二羟基-23-氧代维生素D3(1,25(OH)2-23-氧代-D3)和1α,25,26-三羟基-23-氧代维生素D3(1,25,26(OH)3-23-氧代-D3),以及一种未知代谢产物,其侧链可能已发生修饰/裂解,使得底物中的氚转化为挥发性形式。最近已报道了从雏鸡肠黏膜匀浆中分离和化学鉴定1,25(OH)2-23-氧代-D3和1,25,26(OH)3-23-氧代-D3的过程(大沼直、克鲁斯、波皮雅克和诺曼·A·W.(1982年)《生物化学杂志》257卷,5097 - 510₂页)。基于对雏鸡肠匀浆的动力学研究,提出的C-23氧化途径为:1,25(OH)2D3生成1,25(OH)2-23-氧代-D3,再生成1,25,26(OH)3-23-氧代-D3,最后生成侧链改变的未知代谢产物。维生素D充足的雏鸡组织中C-23途径的相对酶活性为:肠>肾脏>肝脏,比例为18:3:小于1。雏鸡肠黏膜匀浆中C-23途径的活性可通过给鸡静脉注射单次剂量500 ng(1.3 nmol)的1,25(OH)2D3进行预激发而增强10倍;酶活性在3 - 6小时达到最大值,12小时后恢复到基础水平。对雏鸡和大鼠肠匀浆中的这种C-23途径与先前已知的C-24氧化途径进行了比较,后者将1,25(OH)2D3转化为1,24,25-三羟基维生素D3(1,24,25(OH)3D3);据计算,在这些条件下,72%的1,25(OH)2D3通过C-23氧化途径代谢,13%通过C-24途径代谢,只有14%通过其他尚未明确的途径代谢。有人提出,新发现的由靶器官肠黏膜和肾脏对1,25(OH)2D3进行代谢C-23途径,在生理条件下控制这种激素活性形式的维生素D3的组织水平方面可能发挥重要作用。

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