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人类胸腺中肿瘤坏死因子-α和干扰素-γ的表达。唐氏综合征(21三体)中的定位与过表达。

Tumor necrosis factor-alpha and IFN-gamma expression in human thymus. Localization and overexpression in Down syndrome (trisomy 21).

作者信息

Murphy M, Friend D S, Pike-Nobile L, Epstein L B

机构信息

Department of Pediatrics, University of California, San Francisco 94143.

出版信息

J Immunol. 1992 Oct 1;149(7):2506-12.

PMID:1388194
Abstract

In vitro studies suggest that TNF-alpha and IFN-gamma regulate thymocyte proliferation, but little evidence exists for the constitutive production of these cytokines in normal human thymus. In paired experiments, we examined frozen sections of postnatal human thymus from four control children and four age-matched children with Down syndrome (DS) (trisomy 21) for TNF-alpha and IFN-gamma mRNA expression using in situ hybridization. We studied thymuses from children with DS because this aneuploid condition is associated with a greatly increased incidence of infection and has abnormal thymic anatomy and patterns of thymocyte maturation. We found cells expressing constitutive levels of TNF-alpha mRNA in the trabeculae, corticomedullary junctions, and medulla of both control and DS thymuses and the number of these cells was an average of 3.9-fold higher in DS thymuses than in age-matched control thymuses. DS thymuses also contained an average of 3 fold higher numbers of cells with mast cell morphology, identified by toluidine blue histologic staining and electron microscopy. In both DS and control thymuses the mast cells colocalized with TNF-alpha mRNA-expressing cells. In addition, TNF-alpha protein- expressing cells, identified by immunohistochemistry, displayed a granular pattern of staining that is characteristic of mast cells. These results suggest that mast cells may be one source of TNF-alpha in human postnatal thymus. Discrete cells expressing IFN-gamma mRNA were distinctly localized to the cortical region of both DS and control thymuses and were 2.4-fold more abundant in DS thymuses than in the controls. Our results demonstrate, for the first time, the constitutive production and location of TNF-alpha and IFN-gamma in postnatal human thymus. The overexpression of both of these cytokines in DS thymuses suggests a dysregulation in cytokine production in DS and may provide an explanation for the abnormal thymic anatomy and thymocyte maturation associated with this syndrome.

摘要

体外研究表明,肿瘤坏死因子-α(TNF-α)和γ干扰素(IFN-γ)可调节胸腺细胞增殖,但在正常人胸腺中,关于这些细胞因子组成性产生的证据很少。在配对实验中,我们使用原位杂交技术,检测了4名对照儿童和4名年龄匹配的唐氏综合征(DS)(21三体)儿童出生后人胸腺的冷冻切片中TNF-α和IFN-γ mRNA的表达。我们研究了DS患儿的胸腺,因为这种非整倍体状况与感染发生率大幅增加相关,且胸腺解剖结构和胸腺细胞成熟模式异常。我们发现,在对照和DS胸腺的小梁、皮质髓质交界处和髓质中,均有表达TNF-α mRNA组成水平的细胞,且DS胸腺中这些细胞的数量平均比年龄匹配的对照胸腺高3.9倍。DS胸腺中,经甲苯胺蓝组织学染色和电子显微镜鉴定,具有肥大细胞形态的细胞数量平均也高出约3倍。在DS和对照胸腺中,肥大细胞均与表达TNF-α mRNA的细胞共定位。此外,通过免疫组织化学鉴定的表达TNF-α蛋白的细胞呈现出肥大细胞特有的颗粒状染色模式。这些结果表明,肥大细胞可能是人类出生后胸腺中TNF-α的一个来源。表达IFN-γ mRNA的离散细胞明显定位于DS和对照胸腺的皮质区域,且DS胸腺中的此类细胞比对照胸腺多2.4倍。我们的结果首次证明了出生后人胸腺中TNF-α和IFN-γ的组成性产生及其定位。这两种细胞因子在DS胸腺中的过表达表明DS中细胞因子产生存在失调,这可能为与该综合征相关的胸腺解剖结构异常和胸腺细胞成熟异常提供一种解释。

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