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阐明化学变应原处理后树突状细胞表面标志物表达的变化。

Elucidating changes in surface marker expression of dendritic cells following chemical allergen treatment.

作者信息

Hulette Ben A, Ryan Cindy A, Gerberick G Frank

机构信息

The Procter & Gamble Company, Miami Valley Laboratories, Cincinnati, Ohio 45253, USA.

出版信息

Toxicol Appl Pharmacol. 2002 Aug 1;182(3):226-33. doi: 10.1006/taap.2002.9447.

Abstract

Dendritic cells (DC) are highly specialized antigen-presenting cells (APC) located in lymphoid and many nonlymphoid tissues, and Langerhans cells (LC), a specialized form of DC, are found in the skin. LC play a critical role in the induction of contact dermatitis and therefore have become a focal point for the development of in vitro cell-based methods for contact sensitization testing. Because of the low abundance of skin-derived LC, methods to culture DC from peripheral blood are being used by investigators to generate LC surrogates to examine the effects of sensitizing chemicals on APC. It has been reported recently that chemical allergens can induce changes in the expression of various DC surface markers and it has been suggested that the measure of these changes in surface marker expression following allergen treatment could provide the basis for an in vitro test method to predict the contact sensitization potential of a chemical. For the work presented here, DC were differentiated from human peripheral blood mononuclear cells (PBMC-DC) in culture medium containing GM-CSF and interleukin (IL)-4 to ensure an immature phenotype or were derived from the KG-1 cell line (KG-1 DC) using a defined cytokine cocktail consisting of GM-CSF, IL-4, Flt-3/Flk-2-ligand, thrombopoietin, stem cell factor, and tumor necrosis factor-alpha (TNFalpha). Surface marker expression (HLA-DR, CD54, CD80, and CD86) on these DC was measured by flow cytometry after 48 h treatment with the known chemical allergens dinitrofluorobenzene (DNFB) and methylchloroisothiazolinone/methylisothiazolinone (MCI/MI), the irritant sodium dodecyl sulfate, lipopolysaccharide (LPS), and TNFalpha. Treatment of PBMC-DC with either MCI/MI or DNFB induced a slight upregulation of class II major histocompatibility (MHC) expression (HLA-DR), whereas LPS and TNFalpha significantly upregulated CD54 and slightly upregulated CD80 and HLA-DR expression. For KG-1 DC, only MCI/MI upregulated CD86 expression, whereas TNFalpha upregulated CD54 and slightly upregulated CD80 and CD86 expression. SDS had no effect on surface marker expression in either PBMC-DC or KG-1 DC. Changes in surface marker expression in PBMC-DC treated with chemical allergens were detected in two of five donors, suggesting a limited sensitivity of PBMC-DC under these defined isolation and culture conditions. Furthermore, we found that the presence of GM-CSF and IL-4 during chemical allergen treatment masked the ability to detect changes in surface marker expression. Our data suggest that, under these culture and treatment conditions, measurement of surface marker changes in vitro using PBMC-DC or KG-1 DC does not provide a sensitive in vitro method with sufficient dynamic range for assessing the contact sensitization potential of a chemical.

摘要

树突状细胞(DC)是高度特化的抗原呈递细胞(APC),位于淋巴组织和许多非淋巴组织中,而朗格汉斯细胞(LC)是DC的一种特殊形式,存在于皮肤中。LC在接触性皮炎的诱导中起关键作用,因此已成为开发基于细胞的体外接触致敏测试方法的焦点。由于皮肤来源的LC数量稀少,研究人员正在使用从外周血培养DC的方法来生成LC替代物,以研究致敏化学物质对APC的影响。最近有报道称,化学过敏原可诱导各种DC表面标志物表达的变化,有人提出,在过敏原处理后测量这些表面标志物表达的变化可为预测化学物质接触致敏潜力的体外测试方法提供依据。对于此处介绍的工作,DC在含有粒细胞巨噬细胞集落刺激因子(GM-CSF)和白细胞介素(IL)-4的培养基中从人外周血单个核细胞(PBMC-DC)分化而来,以确保未成熟表型,或者使用由GM-CSF、IL-4、Flt-3/Flk-2配体、血小板生成素、干细胞因子和肿瘤坏死因子-α(TNFα)组成的特定细胞因子混合物从KG-1细胞系(KG-1 DC)获得。在用已知化学过敏原二硝基氟苯(DNFB)和甲基氯异噻唑啉酮/甲基异噻唑啉酮(MCI/MI)、刺激性十二烷基硫酸钠、脂多糖(LPS)和TNFα处理48小时后,通过流式细胞术测量这些DC上的表面标志物表达(HLA-DR、CD54、CD80和CD86)。用MCI/MI或DNFB处理PBMC-DC会导致II类主要组织相容性(MHC)表达(HLA-DR)略有上调,而LPS和TNFα会显著上调CD54,并略微上调CD80和HLA-DR表达。对于KG-1 DC,只有MCI/MI上调CD86表达,而TNFα上调CD54,并略微上调CD80和CD86表达。SDS对PBMC-DC或KG-1 DC的表面标志物表达均无影响。在用化学过敏原处理的PBMC-DC中,在五名供体中的两名中检测到表面标志物表达的变化,这表明在这些特定的分离和培养条件下,PBMC-DC的敏感性有限。此外,我们发现化学过敏原处理期间GM-CSF和IL-4的存在掩盖了检测表面标志物表达变化的能力。我们的数据表明,在这些培养和处理条件下,使用PBMC-DC或KG-1 DC体外测量表面标志物变化并不能提供一种灵敏的体外方法,以具有足够的动态范围来评估化学物质的接触致敏潜力。

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