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Transcriptional regulation of caspases in experimental pneumococcal meningitis.

机译:实验性肺炎球菌脑膜炎中胱天蛋白酶的转录调控。

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Apoptosis and necrosis in brain account for neurological sequelae in survivors of bacterial meningitis. In meningitis, several mechanisms may trigger death pathways leading to activation of transcription factors regulating caspases mRNA synthesis. Therefore, we used a multiprobe RNA protection assay (RPA) to examine the expression of 9 caspase-mRNA in the course of experimental Streptococcus pneumoniae meningitis in mouse brain. Caspase-6, -7 and -11 mRNA were elevated 6 hours after infection. 12 hours after infection caspases-1, -2, -8 and -12 mRNA rose. Caspase-14 mRNA was elevated 18 h and caspase-3 mRNA 24 h after infection. In situ hybridization detected caspases-3, -8, -11 and -12 mRNA in neurons of the hippocampal formation and neocortex. Development of sepsis was paralleled by increased transcription of caspases mRNA in the spleen. In TNFalpha-deficient mice all caspases examined were less upregulated, in TNF-receptor 1/2 knockout mice caspases-1, -2, -7, -11 and -14 mRNA were increased compared to infected control animals. In caspase-1 deficient mice, caspases-11, and -12 mRNA levels did not rise in meningitis indicating the necessity of caspase-1 activating these caspases. Hippocampal formations of newborn mice incubated with heat-inactivated S. pneumoniae R6 showed upregulation of caspase-1, -3, -11 and -12 mRNA. These observations suggest a tightly regulated caspases network at the transcriptional level in addition to the known cascade at the protein level.
机译:脑中的细胞凋亡和坏死是细菌性脑膜炎幸存者的神经系统后遗症。在脑膜炎中,多种机制可能触发死亡途径,从而导致调节胱天蛋白酶mRNA合成的转录因子激活。因此,我们在小鼠脑中实验性肺炎链球菌脑膜炎的过程中使用了多探针RNA保护测定(RPA)来检查9 caspase-mRNA的表达。感染后6小时,Caspase-6,-7和-11 mRNA升高。感染后12小时,caspases-1,-2,-8和-12 mRNA升高。感染后18 h,Caspase-14 mRNA升高,而caspase-3 mRNA升高24 h。原位杂交检测海马结构和新皮层神经元中的caspases-3,-8,-11和-12 mRNA。脓毒症的发展与脾中胱天冬氨酸蛋白酶的mRNA转录增加平行。在TNFalpha缺陷型小鼠中,检查的所有胱天蛋白酶均较不上调,在TNF受体1/2敲除小鼠中,胱天蛋白酶-1,-2,-7,-11和-14 mRNA的表达均高于感染的对照动物。在缺乏caspase-1的小鼠中,脑膜炎中caspases-11和-12 mRNA的水平没有升高,表明caspase-1激活这些caspases的必要性。用热灭活的肺炎链球菌R6孵育的新生小鼠海马结构显示caspase-1,-3,-11和-12 mRNA上调。这些观察结果表明,除了已知的蛋白质级联反应外,转录水平上的胱冬酶网络也受到严格调控。

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