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首页> 外文期刊>American Journal of Physiology >Estrogen increases sensitivity of hepatic Kupffer cells to endotoxin.
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Estrogen increases sensitivity of hepatic Kupffer cells to endotoxin.

机译:雌激素增加肝库普弗细胞对内毒素的敏感性。

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摘要

The relationship among gender, lipopolysaccharide (LPS), and liver disease is complex. Accordingly, the effect of estrogen on activation of Kupffer cells by endotoxin was studied. All rats given estrogen intraperitoneally 24 h before an injection of a sublethal dose of LPS (5 mg/kg) died within 24 h, whereas none of the control rats died. Mortality was prevented totally by pretreatment with gadolinium chloride, a Kupffer cell toxicant. Peak serum tumor necrosis factor-alpha (TNF-alpha) values as well as TNF-alpha mRNA in the liver after LPS were twice as high in the estrogen-treated group as in the untreated controls. Plasma nitrite levels and inducible nitric oxide synthase in the liver were also elevated significantly in estrogen-treated rats 6 h after LPS. Furthermore, Kupffer cells isolated from estrogen-treated rats produced about twice as much TNF-alpha and nitrite as controls did in response to LPS. In addition, Kupffer cells from estrogen-treated rats required 15-fold lower amounts of LPS to increase intracellular Ca2+ than controls did, and Kupffer cells from estrogen-treated animals expressed more CD14, the receptor for LPS/LPS binding protein, than controls. Moreover, estrogen treatment increased LPS binding protein mRNA dramatically in liver in 6-24 h. It is concluded that estrogen treatment in vivo sensitizes Kupffer cells to LPS, leading to increased toxic mediator production by the liver.
机译:性别,脂多糖(LPS)和肝病之间的关系很复杂。因此,研究了雌激素对内毒素激活库普弗细胞活化的作用。在注射亚致死剂量的LPS(5 mg / kg)前24小时腹膜内给予雌激素的所有大鼠在24 h内死亡,而对照组大鼠均无死亡。氯化g(一种Kupffer细胞毒物)的预处理可完全防止死亡率。 LPS后,肝脏中的血清肿瘤坏死因子-α(TNF-α)峰值以及肝脏中的TNF-αmRNA在雌激素治疗组中的水平是未治疗对照组的两倍。 LPS后6小时,用雌激素治疗的大鼠肝脏中的血浆亚硝酸盐水平和诱导型一氧化氮合酶也显着升高。此外,从雌激素治疗的大鼠中分离出的库普弗细胞产生的TNF-α和亚硝酸盐约为对照品对LPS的两倍。此外,来自雌激素处理的大鼠的库普弗细胞所需的LPS量要比对照组低15倍,以增加细胞内Ca2 +,而来自雌激素处理的动物的库普弗细胞表达的CD14(LPS / LPS结合蛋白的受体)比对照组更多。此外,雌激素治疗可在6-24小时内显着增加肝脏中LPS结合蛋白的mRNA表达。结论是,体内雌激素治疗可使库普弗细胞对LPS敏感,从而导致肝脏毒性介质的产生增加。

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