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人肥大细胞通过高亲和力IgE受体交联产生白细胞介素-13:白细胞介素-4预处理的人肥大细胞增强白细胞介素-13的产生。

Human mast cells produce IL-13 by high-affinity IgE receptor cross-linking: enhanced IL-13 production by IL-4-primed human mast cells.

作者信息

Toru H, Pawankar R, Ra C, Yata J, Nakahata T

机构信息

Department of Pediatrics, School of Medicine, Tokyo Medical and Dental University, Japan.

出版信息

J Allergy Clin Immunol. 1998 Sep;102(3):491-502. doi: 10.1016/s0091-6749(98)70140-x.

Abstract

BACKGROUND

Mast cells play a central role not only in the early phase of the allergic reaction, but also participate in the late phase of the allergic reaction through the allergen and IgE-dependent release of multifunctional cytokines.

OBJECTIVE

Using the recently established culture system for human mast cells, we examined the expression of a variety of cytokines in cord blood-derived human cultured mast cells (HCMCs) in response to different stimuli.

METHODS

HCMCs were grown from cord blood mononuclear cells in the presence of stem cell factor and IL-6 for 10 weeks. Cytokine mRNA expression in HCMCs by the different stimuli was examined by RT-PCR. Then taking 2 important cytokines, IL-13 and IL4, that share several functional properties and play important roles in allergic diseases, we examined protein as well as mRNA expression of both cytokines in HCMCs.

RESULTS

HCMCs did not express either IL-13 or IL-4 spontaneously. Stimulation with PMA + A23187 induced the expression of IL4 protein, as well as IL-13 protein, in their cytoplasm, although IL-4 secreted in the supernatant was below detectable levels in contrast to a significant amount of IL-13. Stimulation of HCMCs by cross-linking of the high-affinity IgE receptor (Fc(epsilon)RI) induced the expression of IL-13 mRNA and protein, but not IL4. Although we previously found that IL-4 upregulates Fc(epsilon)RI expression on HCMCs, when HCMCs were first cultured in the presence of IL4 and then activated through FC(epsilon)RI cross-linking, remarkable increase was found in IL-13 production. Furthermore, although IL-4 was still undetectable at protein level, IL-4 mRNA expression was induced in the IL-4-primed HCMCs stimulating Fc(epsilon)RI cross-linking. In addition, we examined the effects of these cytokines on the surface molecule expression in HCMCs. Although IL4 remarkably upregulated lymphocyte function-associated antigen-1, intercellular adhesion molecule-1, and Fc(epsilon)RI expression and downregulated c-kit expression in HCMCs, IL-13 did not.

CONCLUSIONS

Our observation that HCMCs produce IL-13 on cross-linking of Fc(epsilon)RI, which was enhanced by IL-4 priming, supports an important role of mast cells in amplification of allergic reaction and further suggests one of the mechanisms enhancing mast cell function in the microenvironment.

摘要

背景

肥大细胞不仅在过敏反应的早期阶段发挥核心作用,还通过变应原和IgE依赖的多功能细胞因子释放参与过敏反应的晚期阶段。

目的

利用最近建立的人肥大细胞培养系统,我们检测了脐血来源的人培养肥大细胞(HCMC)中多种细胞因子在不同刺激下的表达。

方法

在干细胞因子和IL-6存在的情况下,从脐血单个核细胞培养HCMC 10周。通过RT-PCR检测不同刺激下HCMC中细胞因子mRNA的表达。然后选取在过敏疾病中具有多种功能特性并发挥重要作用的两种重要细胞因子IL-13和IL-4,检测它们在HCMC中的蛋白质和mRNA表达。

结果

HCMC不自发表达IL-13或IL-4。用PMA + A23187刺激可诱导其细胞质中IL-IL-13蛋白的表达,尽管与大量的IL-13相比,上清液中分泌的IL-4低于可检测水平。通过高亲和力IgE受体(Fc(ε)RI)交联刺激HCMC可诱导IL-13 mRNA和蛋白的表达,但不能诱导IL-4的表达。尽管我们之前发现IL-4可上调HCMC上Fc(ε)RI的表达,但当HCMC首先在IL-4存在的情况下培养,然后通过Fc(ε)RI交联激活时,发现IL-13的产生显著增加。此外,尽管在蛋白质水平上仍检测不到IL-4,但在刺激Fc(ε)RI交联的IL-4预处理的HCMC中可诱导IL-4 mRNA的表达。另外,我们检测了这些细胞因子对HCMC表面分子表达的影响。尽管IL-4可显著上调HCMC中淋巴细胞功能相关抗原-1、细胞间黏附分子-1和Fc(ε)RI的表达并下调c-kit的表达,但IL-13没有此作用。

结论

我们观察到Fc(ε)RI交联时HCMC产生IL-13,且IL-4预处理可增强这种作用,这支持了肥大细胞在过敏反应放大中的重要作用,并进一步提示了在微环境中增强肥大细胞功能的一种机制。

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