在K14-IL-4 SKH1转基因小鼠模型中,特应性皮炎的发展与免疫球蛋白E上调无关。
The development of atopic dermatitis is independent of Immunoglobulin E up-regulation in the K14-IL-4 SKH1 transgenic mouse model.
作者信息
Chen L, Overbergh L, Mathieu C, Chan L S
机构信息
Department of Dermatology, University of Illinois, Chicago, IL 60612, USA.
出版信息
Clin Exp Allergy. 2008 Aug;38(8):1367-80. doi: 10.1111/j.1365-2222.2008.02987.x. Epub 2008 Apr 13.
BACKGROUND
We have successfully generated an IgE-associated (extrinsic/allergic) mouse model of atopic dermatitis in K14-IL-4-Tg/CByB6 mice. The newly described subset of non-IgE-associated (intrinsic/non-allergic) atopic dermatitis in human patients raises the question on the role of IgE in the pathogenesis.
OBJECTIVE
The aim of this study was to develop a non-IgE-associated atopic dermatitis model in K14-IL-4-Tg/SKH1 mice.
METHODS
K14-IL-4-Tg/CByB6 mice were crossed with SKH1 mice to produce K14-IL-4-Tg/SKH1 mice. Phenotypes of clinical and histological, cytokine expression in the skin lesions, and total serum IgE in K14-IL-4-Tg/CByB6 and K14-IL-4-Tg/SKH1 mice were compared. The CD40 and CD40L on T and B cells were also studied to differentiate their roles in IgE production.
RESULTS
K14-IL-4-Tg/SKH1mice had a normal total serum IgE level and manifested a chronic inflammatory skin phenotype identical to that of K14-IL-4-Tg/CByB6 IgE-mediated mice in clinical morphology, histology, infiltration of mononuclear cells/eosinophils/mast cells, mast cell degranulation, and up-regulation of chronic lesional cytokine mRNA expression of IL-1 beta, IL-3, IL-4, IL-6, IL-10, IL-12, IL-13, IFN-gamma, TNF-alpha, and TNF-beta. We also found that the inability of CD4(+) T cells of the K14-IL-4-Tg/SKH1mice to up-regulate CD40L expression upon stimulation might account for their inability to up-regulate the IgE level. B cell abnormality was ruled out as CD19(+) B cells of K14-IL-4-Tg/SKH1 mice synthesized the same amount of IgE in vitro compared with K14-IL-4-Tg/CByB6 mice in the presence of IL-4 and soluble CD40L. Our studies further suggested that the defect of early growth response-1 in T cells might be responsible for the impaired CD40L up-regulation in K14-IL-4-Tg/SKH1 mice.
CONCLUSION
K14-IL-4-Tg/SKH1 mice developed skin inflammation that resembled human intrinsic atopic dermatitis. Therefore, this model may be suitable to study the pathogenesis of intrinsic atopic dermatitis.
背景
我们已在K14-IL-4-Tg/CByB6小鼠中成功构建了一种与IgE相关(外源性/过敏性)的特应性皮炎小鼠模型。人类患者中新描述的非IgE相关(内源性/非过敏性)特应性皮炎亚组引发了关于IgE在发病机制中作用的问题。
目的
本研究旨在构建一种K14-IL-4-Tg/SKH1小鼠的非IgE相关特应性皮炎模型。
方法
将K14-IL-4-Tg/CByB6小鼠与SKH1小鼠杂交,产生K14-IL-4-Tg/SKH1小鼠。比较K14-IL-4-Tg/CByB6和K14-IL-4-Tg/SKH1小鼠的临床和组织学表型、皮肤病变中的细胞因子表达以及血清总IgE水平。还研究了T细胞和B细胞上的CD40和CD40L,以区分它们在IgE产生中的作用。
结果
K14-IL-4-Tg/SKH1小鼠血清总IgE水平正常,在临床形态学、组织学、单核细胞/嗜酸性粒细胞/肥大细胞浸润、肥大细胞脱颗粒以及IL-1β、IL-3、IL-4、IL-6、IL-10、IL-12、IL-13、IFN-γ、TNF-α和TNF-β慢性病变细胞因子mRNA表达上调方面,表现出与K14-IL-4-Tg/CByB6 IgE介导小鼠相同的慢性炎症皮肤表型。我们还发现,K14-IL-4-Tg/SKH1小鼠的CD4(+) T细胞在受到刺激后无法上调CD40L表达,这可能是它们无法上调IgE水平的原因。排除了B细胞异常,因为在存在IL-4和可溶性CD40L的情况下,K14-IL-4-Tg/SKH1小鼠的CD19(+) B细胞在体外合成的IgE量与K14-IL-4-Tg/CByB6小鼠相同。我们的研究进一步表明,T细胞中早期生长反应-1的缺陷可能是K14-IL-4-Tg/SKH1小鼠中CD40L上调受损的原因。
结论
K14-IL-4-Tg/SKH1小鼠发生了类似于人类内源性特应性皮炎的皮肤炎症。因此,该模型可能适合用于研究内源性特应性皮炎的发病机制。
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