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mRNA expression of TLR4, TLR9 and NF-B in a neonatal murine model of necrotizing enterocolitis

机译:在坏死性小肠结肠炎的新生鼠模型中TLR4,TLR9和NF-B的mRNA表达

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A neonatal model of necrotizing enterocolitis (NEC) in mice was established to examine the role of Toll-like receptors (TLRs) 4 and 9, and of nuclear factor (NF)-B by quantitative detection of their mRNAs in intestinal tissue during the occurrence of NEC, and thus aid in the understanding of the basic pathogenesis of NEC. A total of 50 newborn BALB/c mice (specific pathogen-free level) ranging in age from 7 to 10 days, of either gender, and weighing 4.8-5.4 g were selected and randomly divided into a control and test group, n=25 mice per group. Mice in the control group were kept in the same cage with the mother who fed them, free from any interventions. Mice in the test group were separated from their mother 48 h following birth and placed in an incubator, artificially fed with milk substitutes, and regularly treated with hypoxia and cold stimulation (100% nitrogen anoxia for 90 sec, cold stimulation at 4 degrees C for 10 min, 3 times a day for 3 days) to induce the neonatal NEC. The general state and body weight variations of the mice were recorded, the mice were sacrificed and the intestinal tissue necrosis was evaluated visually, the degree of intestinal injury was determined by histopathological staining, and the mRNA expression levels of intestinal tissue TLR4, TLR9 and NF-B were quantified. Of the 25 mice in the test group, 3 died a natural death and 22 were sacrificed; their general state was worse than that of the mice in the control group, and the body weight variations among them were considerably larger. NEC was confirmed in 12 cases by visual inspection, and the average histological scores of the mice in the test group were 3.5 +/- 0.6, significantly higher than that in the control group (P0.05). The mRNA expression of TLR4 and NF-B in the test group were significantly higher than in the control group. By contrast, the mRNA expression of TLR9 was significantly lower in the test group, and differences were statistically significant (P0.05). Thus, the increased mRNA expression of TLR4 and NF-B, and decreased mRNA expression of TLR9 during NEC may be an important inflammatory mechanism of the disease.
机译:建立了小鼠中坏死性肠核炎(NEC)的新生儿模型,以检查在发生期间在肠组织中的MRNA在肠组织中的定量检测它们的核因子(TLRS)4和9和核因子(NF)-B的作用NEC,从而有助于了解NEC的基本发病机制。选择和称重4.8-5.4g的年龄从7至10天内的50例新生BALB / C小鼠(特异性病原体无菌水平),并随机分为对照组和试验组,n = 25每组老鼠。对照组的小鼠与喂食他们的母亲保持在同一笼子里,没有任何干预措施。试验组的小鼠在出生后与母亲48小时分离,并置于培养箱中,人工喂养牛奶替代品,并定期用缺氧和冷刺激治疗(100%氮缺氧90秒,冷刺激在4℃下冷刺激10分钟,每天3次3天)诱导新生儿NEC。记录小鼠的一般状态和体重变化,处死小鼠并在视觉上评估肠道组织坏死,通过组织病理学染色和肠组织TLR4,TLR9和NF的mRNA表达水平测定肠道损伤程度-b量化。在试验组中的25只小鼠中,3人死于自然死亡,22例被牺牲;它们的一般状态比对照组的小鼠更差,它们之间的体重变化相当大。通过目视检查在12例中确认了NEC,试验组中小鼠的平均组织学分数为3.5 +/- 0.6,显着高于对照组(P <0.05)。测试组中TLR4和NF-B的mRNA表达显着高于对照组。相比之下,试验组的TLR9的mRNA表达显着较低,差异有统计学意义(P <0.05)。因此,在NEC期间,TLR4和NF-B的增加的TLR4和NF-B的表达和TLR9的降低的mRNA表达可能是该疾病的重要炎症机制。

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