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首页> 外文期刊>The Journal of Allergy and Clinical Immunology >Identification of cytokine-regulated genes in human leukocytes in vivo.
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Identification of cytokine-regulated genes in human leukocytes in vivo.

机译:体内人白细胞中细胞因子调节基因的鉴定。

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BACKGROUND: Human polymorphic nuclear granulocytes (PMNs) such as neutrophils and eosinophils play a critical role in mediating inflammatory responses to microbial and parasitic infections. Exposure of these leukocytes to cytokines leads to an amplification of granulocyte effector functions by a mechanism termed "priming." Although many studies have investigated the effects of granulocyte priming, little is known concerning the molecular mechanisms that lead to this phenomenon. OBJECTIVE: The purpose of this study was to identify potential markers for granulocyte priming and thus also to gain further insight into the pathogenesis of inflammatory responses. METHODS: We used a modified differential display technique, random arbitrary primed-PCR to identify genes regulated during the priming of human polymorphic nuclear granulocytes by GM-CSF in vitro. Genes identified were validated by Northern blot analysis of in vitro and in vivo primed leukocytes. RESULTS: Several genes were identified and their expression characterized in vitro. One of these genes, 5-lipoxygenase-activating protein, was also found to be up-regulated in leukocytes isolated after allergen challenge of allergic asthmatic patients. CONCLUSION: The use of differential display technology is a rapid and effective means of identifying genes whose expression is regulated by priming in vitro and in vivo. Further analysis will lead to a better understanding of the priming phenotype and may provide further insight into the pathologic mechanisms of inflammatory processes.
机译:背景:诸如中性粒细胞和嗜酸性粒细胞之类的人类多态核粒细胞(PMN)在介导对微生物和寄生虫感染的炎症反应中起关键作用。这些白细胞与细胞因子的接触导致粒细胞效应功能通过称为“启动”的机制而增强。尽管许多研究已经研究了粒细胞引发的作用,但对于导致这种现象的分子机制知之甚少。目的:本研究的目的是鉴定引发粒细胞的潜在标志物,从而进一步了解炎症反应的发病机理。方法:我们使用改良的差异显示技术,随机任意引物PCR来鉴定GM-CSF在人多态核粒细胞引发过程中调控的基因。鉴定的基因通过体外和体内初免白细胞的Northern印迹分析进行验证。结果:鉴定了几种基因,并在体外对其表达进行了表征。还发现这些基因之一,即5-脂氧合酶激活蛋白,在过敏性哮喘患者的变应原攻击后分离出的白细胞中被上调。结论:差异显示技术的使用是一种快速,有效的方法,可鉴定在体外和体内通过引物调控其表达的基因。进一步的分析将导致对启动表型的更好理解,并可能提供对炎症过程病理机制的进一步了解。

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