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淋巴细胞表面标志物和细胞因子适用于在过敏性接触性皮炎的体外模型中检测和评估皮肤致敏性化学物质的效力:LCSA-ly。

Lymphocyte surface markers and cytokines are suitable for detection and potency assessment of skin-sensitizing chemicals in an in vitro model of allergic contact dermatitis: the LCSA-ly.

机构信息

Institute of Clinical Pharmacology and Toxicology, Charité-Universitätsmedizin Berlin, Charitéplatz 1, 10117, Berlin, Germany.

Department of Dermatology and Allergy, Charité-Universitätsmedizin Berlin, Charitéplatz 1, 10117, Berlin, Germany.

出版信息

Arch Toxicol. 2018 Apr;92(4):1495-1505. doi: 10.1007/s00204-018-2164-5. Epub 2018 Jan 30.

Abstract

Allergic contact dermatitis is a widespread health disorder and occupational skin disease. Hence, screening for contact-sensitizing chemicals is highly relevant to toxicology, dermatology, and occupational medicine. The use of animal tests for this purpose is constrained by ethical considerations, need for high-throughput screening, and legislation (e.g., for cosmetics in the European Union). T cell activation is the final and most specific key event of the "adverse outcome pathway" for skin sensitization and therefore a promising target for the development of in vitro sensitization assays. We present a novel in vitro sensitization assay with a lymphocyte endpoint as an add-on to the loose-fit coculture-based sensitization assay (LCSA): the LCSA-ly. While the LCSA measures dendritic cell activation, the LCSA-ly offers the option for an additional lymphocyte endpoint which can be measured concurrently. We incorporated lymphocytes in our previously established coculture of primary human keratinocytes and monocyte-derived dendritic cells and tested nine substances: five sensitizers [2,4-dinitrochlorobenzene (DNCB) 1.25-15 µmol/l, p-phenylenediamine (PPD) 15.6-125 µmol/l, 2-mercaptobenzothiazole (MBT) 50-1000 µmol/l, coumarin, and resorcinol (both: 250-1500 µmol/l)] and four non-sensitizers (monochlorobenzene, caprylic acid, glycerol, and salicylic acid (all: 125-1000 µmol/l)]. DNCB and MBT increased a subset of IL-23 receptor/IFN-γ receptor 1 (CD119) lymphocytes. DNCB, PPD, and MBT enhanced a subunit of the IL-4 receptor (CD124) and a memory marker (CD44) on lymphocytes. Remarkably, DNCB, PPD, and MBT raised IL-4 concentrations in coculture supernatants while IFN-γ levels decreased, which might point to Th2 activation in vitro. Coumarin, resorcinol, and non-sensitizers did not alter any of the tested surface markers or cytokines. IL-17 was not affected by any of the substances. Relative strength of sensitizers according to lymphocyte markers was DNCB > PPD > MBT, which corresponds to earlier results from the LCSA without lymphocyte endpoint, the murine local lymph node assay, and human data. This study is the first to prove the suitability of lymphocyte surface markers for sensitization testing and potency assessment.

摘要

变应性接触性皮炎是一种广泛存在的健康障碍和职业性皮肤病。因此,对接触致敏化学物质的筛选对毒理学、皮肤病学和职业医学具有重要意义。出于伦理考虑、高通量筛选的需要以及立法(例如,在欧盟中用于化妆品),动物试验在此方面受到限制。T 细胞激活是皮肤致敏的“不良结局途径”的最终和最特异的关键事件,因此是开发体外致敏测定的有前途的靶标。我们提出了一种新型的淋巴细胞终点的体外致敏测定法,作为基于松散共培养的致敏测定法(LCSA)的附加方法:LCSA-ly。虽然 LCSA 测量树突状细胞的激活,但 LCSA-ly 提供了同时测量另一个淋巴细胞终点的选择。我们将淋巴细胞纳入我们之前建立的原代人角质形成细胞和单核细胞衍生的树突状细胞的共培养中,并测试了九种物质:五种致敏剂[2,4-二硝基氯苯(DNCB)1.25-15μmol/l,对苯二胺(PPD)15.6-125μmol/l,2-巯基苯并噻唑(MBT)50-1000μmol/l,香豆素和间苯二酚(均为 250-1500μmol/l)]和四种非致敏剂(单氯苯,辛酸,甘油和水杨酸(均为 125-1000μmol/l)]。DNCB 和 MBT 增加了一组白细胞介素 23 受体/干扰素-γ受体 1(CD119)淋巴细胞。DNCB、PPD 和 MBT 增强了淋巴细胞上白细胞介素 4 受体(CD124)的一个亚基和一个记忆标记物(CD44)。值得注意的是,DNCB、PPD 和 MBT 在共培养上清液中升高了白细胞介素 4 的浓度,而干扰素-γ水平下降,这可能表明体外 Th2 激活。香豆素、间苯二酚和非致敏剂均未改变任何测试的表面标记物或细胞因子。任何物质均未影响白细胞介素 17。根据淋巴细胞标记物,致敏剂的相对强度为 DNCB>PPD>MBT,这与没有淋巴细胞终点的 LCSA、小鼠局部淋巴结测定和人类数据的早期结果一致。这项研究首次证明了淋巴细胞表面标记物用于致敏测试和效力评估的适用性。

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