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首页> 外文期刊>Brain research >Differential expression of pro-inflammatory cytokines, endothelin-1 and nitric oxide synthases in the rat carotid body exposed to intermittent hypoxia
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Differential expression of pro-inflammatory cytokines, endothelin-1 and nitric oxide synthases in the rat carotid body exposed to intermittent hypoxia

机译:间歇性缺氧大鼠颈动脉中促炎细胞因子,内皮素-1和一氧化氮合酶的差异表达

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The enhanced carotid body (CB) chemosensory response to hypoxia induced by chronic intermittent hypoxia (CIH) has been attributed to oxidative stress, which is expected to increase the expression of chemosensory modulators including chemoexcitatory pro-inflammatory cytokines in the CB. Accordingly, we studied the time-course of the changes in the immunohistological expression of TNF-alpha, IL-1beta, IL-6, ET-1, iNOS, eNOS and 3-nitrotyrosine in the CB, along with the progression of enhanced CB chemosensory responses to acute hypoxia in male Sprague-Dawley rats exposed to CIH (5%O_2, 12 times/h per 8 h) for 7, 14 and 21 days. Exposure to CIH for 7 days resulted in a sustained potentiation of CB chemosensory responses to acute hypoxia, which persisted until 21 days of CIH. The chemosensory potentiation was paralleled by an increased 3-nitrotyrosine expression in the CB. On the contrary, CIH produced a transient 2-fold increase of ET-1 immunoreactivity at 7 days, a decrease in eNOS immunoreactivity, and a delayed but progressive increase of TNF-a, IL-1beta and iNOS immunoreactivity, which was not associated with changes in systemic plasma levels or immune cell invasion within the CB. Thus, present results suggest that the local expression of chemosensory modulators and pro-inflammatory cytokines in the CB may have different temporal contribution to the CB chemosensory potentiation induced by CIH.
机译:由慢性间歇性缺氧(CIH)引起的对缺氧的颈动脉体(CB)化学感应增强,已被归因于氧化应激,这有望增加化学感应调节剂(包括化学兴奋促炎性细胞因子)在CB中的表达。因此,我们研究了CB中TNF-α,IL-1beta,IL-6,ET-1,iNOS,eNOS和3-硝基酪氨酸的免疫组织学表达变化的时间过程,以及CB增强的进展雄性Sprague-Dawley大鼠在暴露于CIH(5%O_2,每8小时12次/小时,持续8天,7天,14天和21天)后,对急性缺氧的化学感觉反应。暴露于CIH 7天会导致CB对急性缺氧的化学感应反应持续增强,持续到CIH 21天。化学感应增强与CB中3-硝基酪氨酸表达的增加平行。相反,CIH在7天时使ET-1免疫反应性瞬时增加了2倍,eNOS免疫反应性降低,并且TNF-a,IL-1beta和iNOS免疫反应性延迟但逐渐增加,这与CB中全身血浆水平的变化或免疫细胞的入侵。因此,目前的结果表明,化学感应调节剂和促炎细胞因子在CB中的局部表达可能对CIH诱导的CB化学感应增强具有不同的时间贡献。

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