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镉诱导近交系小鼠肝脏异金属硫蛋白浓度升高。

Cadmium-induced elevation of hepatic isometallothionein concentrations in inbred strains of mice.

作者信息

Kershaw W C, Klaassen C D

机构信息

Department of Pharmacology, Toxicology and Therapeutics, University of Kansas Medical Center, Kansas City 66103.

出版信息

Chem Biol Interact. 1991;78(3):269-82. doi: 10.1016/0009-2797(91)90058-f.

Abstract

Susceptibility to Cd toxicity differs among inbred strains of mice. For example, C3H/He mice are sensitive to Cd-induced hepatotoxicity while DBA/2 mice are resistant. Metallothionein (MT), which in rodents exists predominantly as two isoproteins (MT-I and MT-II), is an important endogenous protein in the detoxication of Cd. The present investigation examines the possibility that strain-dependent susceptibility to Cd-induced liver injury is mediated by an inherited inability to accumulate a specific isoform of MT in response to Cd exposure. Hepatic concentrations of MT-I and MT-II were measured in C3H/He (Cd-sensitive) and DBA/2 (Cd-resistant) mice at various times after the administration of non-toxic (2.5 mumol Cd/kg) to hepatototoxic (80 mumol Cd/kg) dosages of Cd. The concentration of MT-I and MT-II in these strains was similar 24 h after injection of non-hepatotoxic dosages of Cd (10 mumol Cd/kg or less) as well as 6-12 h after a mildly hepatotoxic dose of Cd (20 mumol Cd/kg). The concentration of total MT in liver of Cd-sensitive mice was greater than that present in resistant mice 24-72 h after 20 mumol Cd/kg injection. The data indicates that susceptibility to Cd-induced hepatotoxicity observed in C3H/He mice is not due to a deficit in the induction of a particular isoform of MT.

摘要

小鼠近交系对镉毒性的易感性存在差异。例如,C3H/He小鼠对镉诱导的肝毒性敏感,而DBA/2小鼠具有抗性。金属硫蛋白(MT)在啮齿动物中主要以两种同工蛋白(MT-I和MT-II)的形式存在,是镉解毒过程中的一种重要内源性蛋白质。本研究探讨了镉诱导的肝损伤的品系依赖性易感性是否由遗传决定的无法在接触镉时积累特定同工型MT介导的可能性。在给予无毒(2.5 μmol镉/千克)至肝毒性(80 μmol镉/千克)剂量的镉后,在不同时间测量C3H/He(镉敏感)和DBA/2(镉抗性)小鼠肝脏中MT-I和MT-II的浓度。在注射非肝毒性剂量的镉(10 μmol镉/千克或更低)后24小时以及给予轻度肝毒性剂量的镉(20 μmol镉/千克)后6至12小时,这些品系中MT-I和MT-II的浓度相似。在注射20 μmol镉/千克后24至72小时,镉敏感小鼠肝脏中总MT的浓度高于抗性小鼠。数据表明,C3H/He小鼠中观察到的对镉诱导的肝毒性的易感性并非由于特定同工型MT诱导不足所致。

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