3,5 - 二乙氧羰基 - 1,4 - 二氢可力丁所致肝性卟啉病中肝脏卟啉 - 金属螯合酶活性降低。大鼠和小鼠研究。
Decreased liver activity of porphyrin-metal chelatase in hepatic porphyria caused by 3,5-diethoxycarbonyl-1,4-dihydrocollidine. Studies in rats and mice.
作者信息
De Matteis F, Abbritti G, Gibbs A H
出版信息
Biochem J. 1973 Jul;134(3):717-27. doi: 10.1042/bj1340717.
Abstract
- A difference has been found between rats and mice in their sensitivity to the porphyrogenic effect of drugs. Mice are more sensitive than rats to 3,5-diethoxycarbonyl-1,4-dihydrocollidine, but less sensitive than rats to 2-allyl-2-isopropylacetamide. 2. Use has been made of this difference in sensitivity to ascertain the importance of the decrease of liver porphyrin-metal chelatase activity in porphyria caused by 3,5-diethoxycarbonyl-1,4-dihydrocollidine. Mice, which are more sensitive than rats to the stimulation of 5-aminolaevulinate caused by this drug, are also more sensitive with respect to the decrease of chelatase activity. 3. In both species, after treatment with 3,5-diethoxycarbonyl-1,4-dihydrocollidine, the ratio between chelatase activity and 5-aminolaevulinate activity is linear with respect to the reciprocal of the liver porphyrin concentration. This suggests that under these conditions the degree of porphyrin accumulation depends on the balance between rate of porphyrin formation and rate of porphyrin utilization. 4. Compound SKF 525-A (2-diethylaminoethyl 3,3-diphenylpropylacetate) when given before 3,5-diethoxycarbonyl-1,4-dihydrocollidine prevents the appearance of porphyria in the rat and also largely prevents the decrease of chelatase activity. In the mouse it is much less effective in preventing porphyria and it is almost completely inactive in protecting the chelatase from a decrease in activity. 5. Cycloheximide, when given before 3,5-diethoxycarbonyl-1,4-dihydrocollidine also inhibits the induction of 5-aminolaevulinate synthetase and the appearance of porphyria in the rat, but does not prevent the decrease of chelatase activity. These results suggest that two successive stages can be distinguished in the induction process: a first stage leading to inhibition of haem synthesis and a second stage requiring synthesis of protein in the liver and leading to stimulation of 5-aminolaevulinate synthetase.
摘要
- 已发现大鼠和小鼠对药物致卟啉原效应的敏感性存在差异。小鼠对3,5 - 二乙氧基羰基 - 1,4 - 二氢可力丁比大鼠更敏感,但对2 - 烯丙基 - 2 - 异丙基乙酰胺比大鼠不敏感。2. 利用这种敏感性差异来确定3,5 - 二乙氧基羰基 - 1,4 - 二氢可力丁所致卟啉病中肝脏卟啉 - 金属螯合酶活性降低的重要性。对该药物引起的5 - 氨基酮戊酸刺激比大鼠更敏感的小鼠,对螯合酶活性降低也更敏感。3. 在两个物种中,用3,5 - 二乙氧基羰基 - 1,4 - 二氢可力丁处理后,螯合酶活性与5 - 氨基酮戊酸活性的比值相对于肝脏卟啉浓度的倒数呈线性关系。这表明在这些条件下,卟啉积累的程度取决于卟啉形成速率和卟啉利用速率之间的平衡。4. 化合物SKF 525 - A(2 - 二乙氨基乙基3,3 - 二苯基丙基乙酸酯)在3,5 - 二乙氧基羰基 - 1,4 - 二氢可力丁之前给予时,可防止大鼠出现卟啉病,并且在很大程度上也可防止螯合酶活性降低。在小鼠中,它在预防卟啉病方面效果要差得多,并且在保护螯合酶活性不降低方面几乎完全无效。5. 放线菌酮在3,5 - 二乙氧基羰基 - 1,4 - 二氢可力丁之前给予时,也可抑制大鼠中5 - 氨基酮戊酸合成酶的诱导和卟啉病的出现,但不能防止螯合酶活性降低。这些结果表明,在诱导过程中可区分出两个连续阶段:第一阶段导致血红素合成受到抑制,第二阶段需要肝脏中蛋白质的合成并导致5 - 氨基酮戊酸合成酶受到刺激。
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