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首页> 外文期刊>Archives of Toxicology >Investigations on the estrogenic activity of the metallohormone cadmium in the rat intestine.
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Investigations on the estrogenic activity of the metallohormone cadmium in the rat intestine.

机译:对大鼠肠道钙质藻镉雌激素活性的研究。

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Cadmium (Cd), a toxic heavy metal and an important environmental pollutant, is now also regarded as potential endocrine disruptor. Its estrogenic effects have been examined so far just in classical target tissues, e.g. uterus, and mostly upon intraperitoneal (i.p.) injection of CdCl(2). Yet, estrogen receptors are also expressed in the gut, and food is the main source of cadmium intake in the general population. Therefore, possible estrogenic effects were now investigated in the intestine of ovariectomized Wistar rats after oral short- and long-term administration of CdCl(2) (0.05-4 mg/kg bw on 3 days by gavage and 0.4-9 mg/kg bw for 4 weeks in drinking water) or upon i.p. injection (0.00005-2 mg CdCl(2)/kg bw), and compared to steroid estrogen (estradiol or ethinylestradiol) treated groups. Analysis of Cd in kidneys and small intestine by atomic absorption spectrometry showed dose-dependent increases in tissue levels with rather high Cd concentrations in the gut, both after oral and i.p. administration. Expression of metallothionein (MT1a), a typical metal response parameter, was clearly induced in kidney and small intestine of several CdCl(2) treated groups, but also notably increased by steroid estrogens. Levels of estrogen-regulated genes, i.e. pS2/TFF1, vitamin D receptor (VDR), and estrogen receptor alpha and beta (ER alpha/beta) were studied as parameters of hormonal activity: The intestinal mRNA expression of pS2/TFF1 was significantly decreased in the estrogen reference groups, but also after single i.p. injection and oral long-term administration of CdCl(2). In contrast, the mRNA and protein expression of the VDR were unaffected by long-term administration of Cd via drinking water. We detected expression of ERbeta, but not ERalpha in the small intestine of OVX rats. ERbeta mRNA and protein expression were significantly down-regulated by Cd, similar to the ethinylestradiol reference group. The mRNA expression and immunostaining of proliferating cell nuclear antigen (PCNA), as an index for cell proliferation, revealed decreases after long-term administration of Cd and ethinylestradiol. In summary, cadmium exposure was shown to modulate molecular and functional parameters of estrogenicity in the intestinal tract of OVX rats. As the intestine is known to express predominantly ERbeta, and is an important site of interaction with dietary contaminants, it is indicated to further investigate specific molecular mechanisms of cadmium and estrogen receptor interactions in more detail.
机译:镉(CD),有毒重金属和重要的环保污染物,现在也被视为潜在的内分泌干扰。到目前为止,它仅在古典靶组织中检查了其雌激素效果,例如,子宫,大多数在腹膜内(I.P.)注射CDCl(2)。然而,雌激素受体也在肠道中表达,食物是一般人群中镉摄入的主要来源。因此,现在在口服短期和长期施用CDCl(2)后的卵巢切除的Wistar大鼠的肠肠中研究了可能的雌激素效应(通过饲养3天,0.4-9mg / kg BW饮用水4周)或IP注射(0.00005-2mg CDCl(2)/ kg BW),并与类固醇雌激素(雌二醇或乙炔西二醇)处理的基团进行比较。通过原子吸收光谱法分析肾脏和小肠中的CD和小肠的分析显示剂量依赖性组织水平在肠道中具有相当高的Cd浓度的组织水平,在口服和I.P之后。行政。在几种CDCl(2)个处理基团的肾脏和小肠中,清楚地诱导了金属硫蛋白(MT1a)的表达,肾脏和小肠,但也通过类固醇雌激素显着增加。研究了雌激素调节基因的水平,即PS2 / TFF1,维生素D受体(VDR)和雌激素受体α和β(ERα/β)作为激素活动的参数:PS2 / TFF1的肠mRNA表达显着降低在雌激素参考组中,还在单一IP后注射和口服长期施用CDCl(2)。相反,VDR的mRNA和蛋白表达不受通过饮用水的长期施用CD的影响。我们发现了OVX大鼠小肠中的Erbeta表达,但不是Eralpha。通过Cd显着下调erbeta mRNA和蛋白质表达,类似于乙炔雌二醇参考组。增殖细胞核抗原(PCNA)的mRNA表达和免疫染色作为细胞增殖指数,显露在长期施用CD和乙烯醇二醇后降低。总之,显示镉暴露在OVX大鼠肠道中调节雌激素的分子和功能参数。随着肠道的肠道主要表达Erbeta,并且是与膳食污染物相互作用的重要部位,表明进一步研究了镉和雌激素受体相互作用的特定分子机制。

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