The Embryolethality of Lipopolysaccharide in CD-1 and Metallothionein I-II Null Mice: Lack of a Role for Induced Zinc Deficiency or Metallothionein Induction.

Leazer TM; Daston GP; Keen CL; Rogers JM

首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >The Embryolethality of Lipopolysaccharide in CD-1 and Metallothionein I-II Null Mice: Lack of a Role for Induced Zinc Deficiency or Metallothionein Induction.

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The Embryolethality of Lipopolysaccharide in CD-1 and Metallothionein I-II Null Mice: Lack of a Role for Induced Zinc Deficiency or Metallothionein Induction.

机译：脂多糖在CD-1和金属硫蛋白I-II空小鼠中的胚胎发育性：缺乏诱导锌缺乏或金属硫蛋白诱导的作用。

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Lipopolysaccharide (LPS) is embryolethal in CD-1 mice. LPS induces metallothionein (MT) via cytokines, including TNF-alpha, IL-1, and IL-6, which initiate and maintain the acute phase response. Maternal hepatic MT induction in pregnant rats, by diverse toxicants, can result in maternal hypozincemia and subsequent embryonal zinc (Zn) deficiency. We examined the hypothesis that LPS causes embryo toxicity in CD-1 mice via MT induction and subsequent embryo Zn deficiency by (1) determining whether LPS induces maternal hepatic MT and causes Zn redistribution, (2) assessing the effects of maternal Zn supplementation on LPS developmental toxicity, and (3) assessing the role of MT with MT I-II null mice (MTKO). Timed pregnant CD-1 mice were dosed i.p. with LPS (S. typhimurium) (0.05 mg/kg) on gestation day (gd) 9. Zn supplementation was administered on gd 8 (10 mg/kg, pretreatment) or on gd 9 as a cotreatment (5 or 10 mg/kg). MTKO and wild type (WT) mice were dosed with LPS (0.05 or 0.1 mg/kg) on gd 9, and maternal liver MT and Zn and plasma Zn were measured. In CD-1 mice, maternal hepatic MT was elevated 24 h after LPS treatment, and cotreatment with Zn caused further elevation of MT. Maternal hepatic Zn concentrations paralleled hepatic MT concentrations. Maternal plasma Zn on gd 10 showed no consistent effect of LPS treatment or Zn cotreatment on gd 9. Zn pretreatment (10 mg/kg) on gd 8 did not ameliorate LPS embryolethality, while Zn cotreatment (5 or 10 mg/kg) on gd 9 exacerbated the toxicity of LPS. LPS produced a similar incidence of embryolethality in MTKO and WT strains on gd10. Plasma Zn concentrations were similar in both strains, while hepatic Zn concentrations were significantly higher in WT than in the MTKO strain. In conclusion, while LPS can induce maternal hepatic MT and Zn redistribution in CD-1 mice, this does not appear to be a key mechanism leading to LPS embryotoxicity.

机译：脂多糖（LPS）在CD-1小鼠中具有胚胎致死性。 LPS通过包括TNF-α，IL-1和IL-6在内的细胞因子诱导金属硫蛋白（MT），这些细胞因子引发并维持急性期反应。妊娠大鼠中母体肝脏MT的多种毒物诱导可导致母体低锌血症和随后的胚胎锌（Zn）缺乏症。我们检查了以下假设：LPS通过（1）确定LPS是否诱导母体肝MT并引起锌重新分布，（2）评估母体补锌对LPS的影响，通过MT诱导和随后的锌缺乏症在CD-1小鼠中引起胚胎毒性。（3）评估MT与MT I-II无效小鼠（MTKO）的作用。定时给怀孕的CD-1小鼠腹膜内给药。在妊娠第9天用LPS（鼠伤寒沙门氏菌）（0.05 mg / kg）进行补锌。在第8 gd（10 mg / kg，预处理）或第9 gd的补锌（5或10 mg / kg）中施用锌补充剂）。在gd 9上给MTKO和野生型（WT）小鼠服用LPS（0.05或0.1 mg / kg），并测量母体肝脏MT和Zn以及血浆Zn。在CD-1小鼠中，LPS治疗后24小时母体肝脏MT升高，而与Zn的共同治疗导致MT进一步升高。孕妇肝中锌的浓度与肝中MT的浓度平行。 gd 10的母体血浆Zn对gd 9没有显示出LPS处理或锌共处理的一致效果。gd 8上的Zn预处理（10 mg / kg）不能改善LPS胚胎致死性，而gd上的Zn共处理（5或10 mg / kg） 9加剧了LPS的毒性。 LPS在gd10的MTKO和WT菌株中产生了类似的胚胎致死率。两种菌株的血浆锌浓度相似，而野生型的肝锌浓度显着高于MTKO株。总之，虽然LPS可以诱导CD-1小鼠的母体肝MT和Zn再分布，但这似乎不是导致LPS胚胎毒性的关键机制。

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《Toxicological sciences: An official journal of the Society of Toxicology 》 |2003年第2期| 共6页
作者
Leazer TM; Daston GP; Keen CL; Rogers JM;
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正文语种 eng
中图分类药学 ;
关键词
Zinc measurement; Lipopolysaccharides; Metastatic to; Diagnosis; clinical; 脂多糖类;

机译：Zinc measurement;Lipopolysaccharides;Metastatic to;Diagnosis;clinical;脂多糖类;

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1. The Embryolethality of Lipopolysaccharide in CD-1 and Metallothionein I-II Null Mice: Lack of a Role for Induced Zinc Deficiency or Metallothionein Induction. [J] . Leazer TM, Daston GP, Keen CL, Toxicological sciences: An official journal of the Society of Toxicology . 2003 ,第2期

机译：脂多糖在CD-1和金属硫蛋白I-II空小鼠中的胚胎发育性：缺乏诱导锌缺乏或金属硫蛋白诱导的作用。
2. Zinc Pretreatment Inhibits Isotretinoin Teratogenicity and Induces Embryonic Metallothionein in CD-1 Mice [J] . Danielle Blain*, Stan Kubow*, Hing Man Chan*?3 The Journal of Nutrition: Official Organ of the American Institute of Nutrition . 1998 ,第7期

机译：锌预处理抑制异维A酸致畸，并诱导CD-1小鼠胚胎金属硫蛋白。
3. The role of the pancreas in intestinal zinc secretion in metallothionein-null mice. [J] . Rofe AM, Winters N, Hinskens B, Pancreas . 1999 ,第1期

机译：胰腺在金属硫蛋白缺失小鼠中肠道锌分泌的作用。
4. Mutations in C57BI/6J and Metallothionein Knock-out Mice Induced by Chronic Exposure of Sodium Arsenate in Drinking Water [C] . Li, Arungundrum S. Prakash, Michael R. Moore, International conference on arsenic exposure and health effects . 2001

机译：C57Bi / 6J中的突变和饮用水中钠砷酸钠慢性暴露诱导的金属硫蛋白敲除小鼠
5. Effects of marginal zinc deficiency and zinc supplementation on lead toxicity, metallothionein and skeletal development in growing rats. [D] . Jamieson, Jennifer Annette. 2006

机译：边际锌缺乏和补锌对成年大鼠铅毒性，金属硫蛋白和骨骼发育的影响。
6. Hepatic zinc in metallothionein-null mice following zinc challenge: in vivo and in vitro studies. [O] . P Coyle, J C Philcox, A M Rofe 1995

机译：锌激发后无金属硫蛋白的小鼠中的肝锌：体内和体外研究。
7. The Embryolethality of Lipopolysaccharide in CD-1 and Metallothionein I-II Null Mice: Lack of a Role for Induced Zinc Deficiency or Metallothionein Induction [O] . Tyra M. Leazer, George P. Daston, Carl L. Keen, 2002

机译：CD-1和金属硫蛋白I-II空小鼠中脂多糖的胚胎发育：缺乏诱导锌缺乏或金属硫蛋白诱导的作用
8. Altered Zinc Homeostasis and Hepatic Accumulation of Metallothionein in Indomethacin-Induced Enteropathy. [R] . Sobocinski, P. Z., Knutsen, G. L., Canterbury, W. J., 1978

机译：改变吲哚美辛诱导的肠病中锌稳态和金属硫蛋白的肝脏积累。

The Embryolethality of Lipopolysaccharide in CD-1 and Metallothionein I-II Null Mice: Lack of a Role for Induced Zinc Deficiency or Metallothionein Induction.

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