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多胺的相互转化、分解代谢及消除

Interconversion, catabolism and elimination of the polyamines.

作者信息

Seiler N, Bolkenius F N, Rennert O M

出版信息

Med Biol. 1981 Dec;59(5-6):334-46.

PMID:7040832
Abstract

Two catabolic pathways exist for spermidine and spermine. One is responsible for the interconversion of the polyamines, a physiological intracellular event. The first and probably rate limiting step of the polyamine interconversion pathway is acetylation in the N1-position by a cytosolic enzyme. The reaction products N1-acetylspermine and N1-acetylspermidine are substrates of the cytoplasmic polyamine oxidase. This enzyme transforms the N1-acetylpolyamines into spermidine and putrescine respectively. N1-Acetylspermidine is at the same time a major urinary excretion product. The factors which control the rates of N1-acetylspermidine degradation by polyamine oxidase versus its elimination via transport are not known. The second catabolic pathway forms putreanine from spermidine and N8-(2-carboxyethyl)-spermidine and spermic acid from spermine. It is catalyzed by the well known serum spermine oxidase. The second step in this reaction sequence, the dehydrogenation of the aldehydes formed by the serum spermine oxidase occurs intracellularly and is catalyzed either by specific or non-specific aldehyde dehydrogenases. The function of this "two compartment reaction sequence" is most probably to protect tissues from extracellular or exogenous (alimentary) polyamines. Its end-products appear to be physiologically indifferent urinary excretion products. Both catabolic pathways may have marked effects on the urinary polyamine pattern. Drugs as well as a variety of physiological and pathological states may influence polyamine catabolism and elimination at various levels, and may cause characteristic alterations in the urinary excretion of free and conjugated polyamines and of the amino acids deriving from the polyamines.

摘要

亚精胺和精胺存在两种分解代谢途径。一种负责多胺的相互转化,这是一种生理性的细胞内事件。多胺相互转化途径的第一步且可能是限速步骤是由一种胞质酶在N1位进行乙酰化。反应产物N1 - 乙酰精胺和N1 - 乙酰亚精胺是细胞质多胺氧化酶的底物。该酶分别将N1 - 乙酰多胺转化为亚精胺和腐胺。N1 - 乙酰亚精胺同时也是主要的尿排泄产物。控制多胺氧化酶降解N1 - 乙酰亚精胺的速率与其通过转运消除的速率的因素尚不清楚。第二条分解代谢途径由亚精胺形成腐胺宁,由精胺形成N8 - (2 - 羧乙基) - 亚精胺和精胺酸。它由著名的血清精胺氧化酶催化。该反应序列的第二步,即血清精胺氧化酶形成的醛的脱氢反应在细胞内发生,由特异性或非特异性醛脱氢酶催化。这种“双室反应序列”的功能很可能是保护组织免受细胞外或外源性(食物性)多胺的影响。其终产物似乎是生理上无活性的尿排泄产物。两条分解代谢途径都可能对尿多胺模式产生显著影响。药物以及各种生理和病理状态可能在不同水平影响多胺的分解代谢和消除,并可能导致游离和结合多胺以及源自多胺的氨基酸的尿排泄出现特征性改变。

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