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首页> 外文期刊>Toxicology: An International Journal Concerned with the Effects of Chemicals on Living Systems >Endotoxin pretreatment protects against the hepatotoxicity of acetaminophen and carbon tetrachloride: role of cytochrome P450 suppression.
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Endotoxin pretreatment protects against the hepatotoxicity of acetaminophen and carbon tetrachloride: role of cytochrome P450 suppression.

机译:内毒素预处理可防止对乙酰氨基酚和四氯化碳的肝毒性:细胞色素P450抑制作用。

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摘要

Bacterial endotoxin (lipopolysaccharide, LPS) is known to potentiate the toxicity of many hepatotoxicants. However, exposure to a sublethal dose of LPS renders animals tolerant to a lethal dose of LPS, and protects against the toxicity of some chemicals. This study was designed to examine the effects of LPS pretreatment on acetaminophen- and carbon tetrachloride (CCl(4))-induced liver injury in LPS-sensitive C3H/OuJ and LPS-resistant C3H/HeJ mice. Pretreatment of male C3H/OuJ mice with a single injection of LPS (0. 1 mg/kg, ip, for 24 h) protected against the hepatotoxic effects of acetaminophen (400 mg/kg) and carbon tetrachloride (CCl(4), 30 mg/kg), as indicated by serum alanine aminotransferase activity. In contrast, pretreatment of C3H/HeJ mice with 0.1 or 10 mg/kg LPS afforded no protection against the hepatotoxic effects of acetaminophen and CCl(4). In an attempt to determine the mechanism of LPS-induced protection against acetaminophen- and CCl(4)-induced hepatotoxicity in C3H/OuJ mice, liver cytochrome P450 was determined 24 h after LPS injection. LPS treatment caused a 26% decrease in total P450 content in C3H/OuJ but not in C3H/HeJ mice. CYP3A-catalized testosterone 6 beta-, 2 beta-, and 15 beta-hydroxylation was decreased 40% by LPS only in C3H/OuJ mice. To determine whether the differences to LPS-response in the two stains of mice is mediated by a strain-related difference in the release of cytokines, mice were pretreated with interleukin-1 (IL-1 alpha, 5 x 10(5) U/mouse), and the hepatoprotection and hepatic P450 enzymes were examined. IL-1 alpha pretreatment equally protected against the hepatotoxicity of acetaminophen and CCl(4) in both strains, and suppressed the total microsomal P450 and P450 enzyme-catalyzed testosterone hydroxylation to a similar extent. In conclusion, LPS pretreatment suppressed hepatic cytochrome P450 enzymes and protected against the hepatotoxicity of acetaminophen and CCl(4) in LPS-sensitive C3H/OuJ mice, but not in LPS-refractory C3H/HeJ mice. This protective effect of LPS appears to be mediated through the release of cytokines such as IL-1 alpha, which in turn suppresses the cytochrome P450 responsible for the activation of acetaminophen and CCl(4) to reactive metabolites.
机译:已知细菌内毒素(脂多糖,LPS)可增强许多肝毒物的毒性。但是,暴露于亚致死剂量的LPS会使动物耐受致命的LPS剂量,并防止某些化学药品的毒性。本研究旨在检查LPS预处理对LPS敏感的C3H / OuJ和LPS耐药的C3H / HeJ小鼠的对乙酰氨基酚和四氯化碳(CCl(4))诱导的肝损伤的影响。单次注射LPS(0.1 mg / kg,ip,24小时)预处理雄性C3H / OuJ小鼠免受对乙酰氨基酚(400 mg / kg)和四氯化碳(CCl(4),30 mg / kg),如血清丙氨酸氨基转移酶活性所指示。相反,用0.1或10 mg / kg LPS预处理C3H / HeJ小鼠不能抵抗对乙酰氨基酚和CCl(4)的肝毒性作用。为了确定LPS诱导的对乙酰氨基酚和CCl(4)诱导的C3H / OuJ小鼠肝毒性的保护机制,LPS注射后24小时测定了肝细胞色素P450。 LPS处理可使C3H / OuJ小鼠的总P450含量降低26%,但对C3H / HeJ小鼠却没有。 CYP3A催化的睾丸激素6β-,2β-和15β-羟基化仅通过LPS在C3H / OuJ小鼠中降低40%。为了确定两种染色剂对LPS反应的差异是否是由菌株相关的细胞因子释放差异所介导的,对小鼠进行了白介素-1(IL-1 alpha,5 x 10(5)U /小鼠),并检查其肝保护和肝P450酶。 IL-1 alpha预处理同样可防止对乙酰氨基酚和CCl(4)在两个菌株中的肝毒性,并在相似的程度上抑制了总微粒体P450和P450酶催化的睾丸激素羟基化。总之,LPS预处理抑制了LPS敏感的C3H / OuJ小鼠的肝细胞色素P450酶并保护了对乙酰氨基酚和CCl(4)的肝毒性,但对LPS难治的C3H / HeJ小鼠却没有。 LPS的这种保护作用似乎是通过释放诸如IL-1α的细胞因子来介导的,IL-1 alpha进而抑制了负责激活对乙酰氨基酚和CCl(4)到反应性代谢产物活化的细胞色素P450。

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