class='kwd-title'>Abbreviations: ERGs, estrogen '/> Soy supplementation: Impact on gene expression in different tissues of ovariectomized rats and evaluation of the rat model to predict (post)menopausal health effect
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Soy supplementation: Impact on gene expression in different tissues of ovariectomized rats and evaluation of the rat model to predict (post)menopausal health effect

机译:补充大豆:对去卵巢大鼠不同组织中基因表达的影响以及评估预测绝经(后)健康影响的大鼠模型的评估

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class="kwd-title">Abbreviations: ERGs, estrogen responsive genes; ERα, estrogen receptor alpha; ERβ, estrogen receptor beta; PBMC, peripheral blood mononuclear cells class="kwd-title">Keywords: Gene expression, Ovariectomized rat model, (Post)menopausal health effect, Soy isoflavone supplementation class="head no_bottom_margin" id="abs0015title">AbstractThis toxicogenomic study was conducted to predict (post)menopausal human health effects of commercial soy supplementation using ovariectomized rats as a model. Different target tissues (i.e. breast, uterus and sternum) and non-target tissues (i.e. peripheral blood mononuclear cells (PBMC), adipose and liver) of ovariectomized F344 rats exposed to a commercially available soy supplement for eight weeks, were investigated. Changes in gene expression in these tissues were analysed using whole-genome microarray analysis. No correlation in changes in gene expression were observed among different tissues, indicating tissue specific effects of soy isoflavone supplementation. Out of 87 well-established estrogen responsive genes (ERGs), only 19 were found to be significantly regulated (p < 0.05) in different tissues, particularly in liver, adipose and uterus tissues. Surprisingly, no ERGs were significantly regulated in estrogen sensitive breast and sternum tissues. The changes in gene expression in PBMC and adipose tissue in rats were compared with those in (post)menopausal female volunteers who received the same supplement in a similar oral dose and exposure duration in human intervention studies. No correlation in changes in gene expression between rats and humans was observed. Although receiving a similar dose, in humans the plasma levels expressed as total free aglycones were several folds higher than in the rat. Therefore, the overall results in young ovariectomized female F344 rats indicated that using rat transcriptomic data does not provide a suitable model for human risk or benefit analysis of soy isoflavone supplementation.
机译:<!-fig ft0-> <!-fig @ position =“ anchor” mode =文章f4-> <!-fig mode =“ anchred” f5-> <!-fig / graphic | fig / alternatives / graphic mode =“ anchored” m1-> class =“ kwd-title”>缩写: ERGs,雌激素反应性基因; ERα,雌激素受体α; ERβ,雌激素受体β; PBMC,外周血单核细胞 class =“ kwd-title”>关键字:基因表达,去卵巢大鼠模型,绝经后的健康作用,大豆异黄酮补充剂 class =“ head no_bottom_margin” id =“该毒物基因组研究旨在使用去卵巢大鼠作为模型来预测商业大豆补充对绝经后人类健康的影响。研究了暴露于市售大豆补充品中八周的去卵巢F344大鼠的不同目标组织(即乳房,子宫和胸骨)和非目标组织(即外周血单核细胞(PBMC),脂肪和肝)。使用全基因组微阵列分析分析了这些组织中基因表达的变化。在不同组织之间未观察到基因表达变化的相关性,表明大豆异黄酮补充的组织特异性作用。在87种成熟的雌激素反应基因(ERG)中,只有19种在不同组织,特别是肝脏,脂肪和子宫组织中被显着调节(p <0.05)。令人惊讶的是,在雌激素敏感的乳房和胸骨组织中没有ERG被显着调节。在人类干预研究中,将大鼠PBMC和脂肪组织中基因表达的变化与绝经后(女性)志愿者(以相似的口服剂量和暴露时间接受了相同的补充剂)进行了比较。没有观察到大鼠和人类之间基因表达变化的相关性。尽管接受的剂量相似,但在人体中以总游离糖苷配基表达的血浆水平却比大鼠高出几倍。因此,年轻的卵巢切除雌性F344大鼠的总体结果表明,使用大鼠转录组数据不能为补充大豆异黄酮的人类风险或收益分析提供合适的模型。

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