Intestinal NF-κB is activated, mainly as p50 homodimers, by platelet-activating factor

Isabelle G. De Plaen , Xiao-Di Tan , Hong Chang , Xiao-Wu Qu , Qian-Ping Liu , Wei Hsueh
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引用次数: 50

Abstract

NF-κB, a transcription factor, upregulates gene transcription of many inflammatory mediators. Here, we examined the activity of NF-κB in the rat small intestine, and how it may be affected by platelet-activating factor (PAF), an important mediator for intestinal injury and inflammation. Ileal nuclear extracts from sham-operated and PAF (1.5 μg/kg)-injected rats were prepared for the assessment of NF-κB DNA-binding activity, and the identification of NF-κB subunits. The experiment was also performed on neutrophil-depleted rats to examine whether the PAF effect is neutrophil-dependent. Cellular NF-κB was localized by immunohistochemistry. We found that: (a) NF-κB is constitutively active in rat small intestine; (b) PAF at a dose below that causing shock and bowel necrosis enhances DNA-binding activity of NF-κB within 30 min after injection; activated NF-κB contains predominantly p50 subunits; (c) immunohistochemistry showed that PAF induced translocation of p50 into the nucleus of cells of the lamina propria, as well as of the epithelium; and (d) the effect of PAF is abrogated by neutrophil depletion, suggesting a role of neutrophils in NF-κB activation. Our study suggests that NF-κB is weakly active constitutively in the intestine, and inflammatory stimuli such as PAF activate NF-κB and enhance its DNA-binding activity in the intestine, which contains predominantly p50 subunits.

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肠道NF-κB主要以p50同型二聚体的形式被血小板活化因子激活
NF-κB是一种转录因子,可上调许多炎症介质的基因转录。在这里,我们研究了大鼠小肠中NF-κB的活性,以及它如何受到血小板活化因子(PAF)的影响,PAF是肠道损伤和炎症的重要介质。制备假手术大鼠回肠核提取物和注射PAF (1.5 μg/kg)大鼠回肠核提取物,检测NF-κB dna结合活性,鉴定NF-κB亚基。实验还对中性粒细胞缺失的大鼠进行了实验,以检验PAF的作用是否依赖于中性粒细胞。免疫组化法定位细胞NF-κB。我们发现:(a) NF-κB在大鼠小肠中具有组成性活性;(b)注射后30min内,低于致休克和肠坏死剂量的PAF可增强NF-κB的dna结合活性;活化的NF-κB主要含有p50亚基;(c)免疫组化显示PAF诱导p50易位到固有层细胞核和上皮内;(d)中性粒细胞耗竭消除了PAF的作用,提示中性粒细胞在NF-κB活化中的作用。我们的研究表明,NF-κB在肠道中组成性活性较弱,炎症刺激如PAF激活NF-κB并增强其在肠道中的dna结合活性,其中主要含有p50亚基。
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