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通过硫酸化的外源化合物使大鼠肝脏中的3'-磷酸腺苷5'-磷酸硫酸酯(PAPS)和硫酸盐耗竭。

Depletion of hepatic 3'-phosphoadenosine 5'-phosphosulfate (PAPS) and sulfate in rats by xenobiotics that are sulfated.

作者信息

Kim H J, Cho J H, Klaassen C D

机构信息

Department of Pharmacology, Toxicology and Therapeutics, University of Kansas Medical Center, Kansas City, USA.

出版信息

J Pharmacol Exp Ther. 1995 Nov;275(2):654-8.

PMID:7473151
Abstract

Sulfation is considered a high-affinity but low-capacity conjugation mechanism that is limited by the availability of 3'-phosphoadenosine 5'-phosphosulfate (PAPS), the cosubstrate for sulfation. Salicylamide, phenol and 1-naphthol are all known substrates for the sulfation reaction. This study was conducted to determine whether the xenobiotics that are sulfated when administered to rats will lower hepatic PAPS and its precursor, sulfate. Urinary sulfate excretion was reduced 85% to 95% by these compounds. Hepatic PAPS was reduced 73%, 39%, and 87% by salicylamide, phenol and naphthol, respectively, 2 hr after administration of 2 mmol/kg. These compounds also decreased serum sulfate concentrations by 45% to 86% and lowered hepatic sulfate concentrations. In summary, these studies demonstrate that salicylamide, phenol and 1-naphthol lower hepatic PAPS and sulfate concentrations, as well as serum sulfate concentrations. These findings imply that increased sulfation, as a result of the sulfation of xenobiotics, results in depletion of hepatic PAPS concentrations, possibly because the utilization of PAPS by the sulfotransferases exceeds its generation via sulfate activation. Thus the capacity-limited sulfation of high dosages of xenobiotics appears to be due to the reduced availability of hepatic PAPS, which in turn is limited by the availability of sulfate.

摘要

硫酸化被认为是一种高亲和力但低容量的结合机制,它受到硫酸化的共底物3'-磷酸腺苷5'-磷酸硫酸酯(PAPS)可用性的限制。水杨酰胺、苯酚和1-萘酚都是硫酸化反应的已知底物。本研究旨在确定给予大鼠时会发生硫酸化的外源性物质是否会降低肝脏中的PAPS及其前体硫酸盐。这些化合物使尿中硫酸盐排泄减少了85%至95%。给予2 mmol/kg后2小时,水杨酰胺、苯酚和萘酚分别使肝脏PAPS降低了73%、39%和87%。这些化合物还使血清硫酸盐浓度降低了45%至86%,并降低了肝脏硫酸盐浓度。总之,这些研究表明水杨酰胺、苯酚和1-萘酚会降低肝脏PAPS和硫酸盐浓度以及血清硫酸盐浓度。这些发现意味着,由于外源性物质的硫酸化导致硫酸化增加,会导致肝脏PAPS浓度耗尽,这可能是因为硫酸转移酶对PAPS的利用超过了其通过硫酸盐活化的生成。因此,高剂量外源性物质的容量受限硫酸化似乎是由于肝脏PAPS可用性降低,而这又受到硫酸盐可用性的限制。

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