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通过单细胞PCR分析人结肠黏膜FcεRI阳性细胞中的细胞因子谱:类固醇治疗的炎症性肠病患者中IL-3表达的抑制

Analysis of cytokine profile in human colonic mucosal Fc epsilonRI-positive cells by single cell PCR: inhibition of IL-3 expression in steroid-treated IBD patients.

作者信息

Ligumsky M, Kuperstein V, Nechushtan H, Zhang Z, Razin E

机构信息

Division of Internal Medicine, Hadassah Medical Center, Jerusalem, Israel.

出版信息

FEBS Lett. 1997 Aug 25;413(3):436-40. doi: 10.1016/s0014-5793(97)00933-2.

DOI:10.1016/s0014-5793(97)00933-2
PMID:9303551
Abstract

Mast cells can serve as a possible important source of cytokine production in inflamed tissue which can be regulated by stimuli different from those activating other immune system cells. To study the expression of specific genes in mast cells derived from small human colonic mucosal endoscopic biopsies, we first modified a previously reported procedure to achieve a significantly enriched mast cell fraction. Then, by using single-cell RT-PCR analysis the expression of the IgE Fc receptor (Fc epsilonRI) and c-kit mRNA was determined. It was observed that the Fc epsilonRI-positive cells also expressed c-kit. This observation provided further evidence that Fc epsilonRI-positive cells are indeed mast cells. Analysis of biopsies from 12 patients (four control and eight patients with inflammatory bowel disease (IBD)) was carried out, revealing that all of the Fc epsilonRI-positive cells expressed IL-3, while the expression of IL-4 was detected only in some of these positive cells. TNF alpha was not detected in these cells. Therefore, it would seem that most intestinal mast cells produce IL-3. Since it has been reported that IL-3 synthesis was down-regulated in steroid-treated cells, the expression pattern of IL-3 in intestinal mast cells derived from steroid-treated IBD patients was then determined. IL-3 mRNA was detected in only two out of 24 Fc epsilonRI-positive cells derived from these steroid-treated patients. These results lend strong support to the idea that the down-regulation of IL-3 in mast cells derived from steroid-treated IBD patients occurs in vivo and could be an important mechanism for immunomodulation in IBD.

摘要

肥大细胞可能是炎症组织中细胞因子产生的一个重要来源,其可由不同于激活其他免疫系统细胞的刺激所调控。为了研究源自人结肠黏膜内镜活检小样本的肥大细胞中特定基因的表达,我们首先改进了先前报道的方法,以获得显著富集的肥大细胞组分。然后,通过单细胞逆转录聚合酶链反应(RT-PCR)分析,测定了IgE Fc受体(FcεRI)和c-kit mRNA的表达。观察到FcεRI阳性细胞也表达c-kit。这一观察结果进一步证明FcεRI阳性细胞确实是肥大细胞。对12例患者(4例对照和8例炎症性肠病(IBD)患者)的活检样本进行分析,结果显示所有FcεRI阳性细胞均表达IL-3,而仅在部分阳性细胞中检测到IL-4的表达。这些细胞中未检测到肿瘤坏死因子α(TNFα)。因此,似乎大多数肠道肥大细胞产生IL-3。由于已有报道称类固醇处理的细胞中IL-3合成下调,则随后测定了源自类固醇处理的IBD患者的肠道肥大细胞中IL-3的表达模式。在源自这些类固醇处理患者的24个FcεRI阳性细胞中,仅在2个细胞中检测到IL-3 mRNA。这些结果有力地支持了以下观点:类固醇处理的IBD患者来源的肥大细胞中IL-3的下调在体内发生,并且可能是IBD免疫调节的重要机制。

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Analysis of cytokine profile in human colonic mucosal Fc epsilonRI-positive cells by single cell PCR: inhibition of IL-3 expression in steroid-treated IBD patients.通过单细胞PCR分析人结肠黏膜FcεRI阳性细胞中的细胞因子谱:类固醇治疗的炎症性肠病患者中IL-3表达的抑制
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