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FADS小鼠:一种新型的特应性角结膜炎小鼠模型。

The FADS mouse: A novel mouse model of atopic keratoconjunctivitis.

作者信息

Nunomura Satoshi, Kitajima Isao, Nanri Yasuhiro, Kitajima Midori, Ejiri Naoko, Lai I-Shuan, Okada Naoko, Izuhara Kenji

机构信息

Division of Medical Biochemistry, Saga Medical School, Saga, Japan.

Department of Clinical Laboratory and Molecular Pathology, Graduate School of Medical and Pharmaceutical Science, Toyama, Japan.

出版信息

J Allergy Clin Immunol. 2021 Dec;148(6):1596-1602.e1. doi: 10.1016/j.jaci.2021.05.017. Epub 2021 May 25.

Abstract

BACKGROUND

Atopic keratoconjunctivitis (AKC) is a chronic allergic conjunctival disease. However, a mouse model of AKC to investigate the underlying mechanism of the therapeutic agents and estimate their efficacy has not been established. We recently generated mice in which Ikk2 is specifically deleted in facial skin fibroblasts and found that these mice spontaneously develop atopic dermatitis (AD)-like facial skin inflammation and scratching behaviors; thus, we named them facial AD with scratching (FADS) mice.

OBJECTIVE

We sought to evaluate whether the ocular lesions that FADS mice spontaneously develop are similar to those of patients with AKC and to estimate the efficacy of topical treatments with tacrolimus and betamethasone for FADS mice by using tear periostin, a novel biomarker for allergic conjunctival disease.

METHODS

FADS mice, in which Ikk2 is deleted in dermal fibroblasts, were generated by crossing female Ikk2 mice to male Nestin; Ikk2 mice. We conducted histologic analysis of the ocular lesions in FADS mice. Furthermore, we measured periostin in the tears collected from FADS mice untreated or treated with tacrolimus or betamethasone.

RESULTS

The FADS mice exhibited severe blepharitis and scratch behaviors for their faces. In these mice, corneal epithelium and stroma showed hyperplasia and infiltration of eosinophils, mast cells, and T2/T2 cells. Periostin was significantly expressed in the lesions and tear periostin was upregulated. Betamethasone showed more suppressive effects than did tacrolimus on severe corneal lesions and increased tear periostin level.

CONCLUSIONS

The FADS mouse is a novel mouse model of AKC and is useful to examine the therapeutic effects of anti-AKC agents.

摘要

背景

特应性角结膜炎(AKC)是一种慢性过敏性结膜疾病。然而,尚未建立用于研究治疗药物潜在机制并评估其疗效的AKC小鼠模型。我们最近培育出了在面部皮肤成纤维细胞中特异性缺失Ikk2的小鼠,发现这些小鼠会自发出现类特应性皮炎(AD)的面部皮肤炎症和抓挠行为;因此,我们将它们命名为伴抓挠的面部AD(FADS)小鼠。

目的

我们试图评估FADS小鼠自发出现的眼部病变是否与AKC患者的病变相似,并通过使用泪液骨膜蛋白(一种用于过敏性结膜疾病的新型生物标志物)来评估他克莫司和倍他米松局部治疗FADS小鼠的疗效。

方法

通过将雌性Ikk2小鼠与雄性巢蛋白-Ikk2小鼠杂交,培育出在真皮成纤维细胞中缺失Ikk2的FADS小鼠。我们对FADS小鼠的眼部病变进行了组织学分析。此外,我们测量了未经治疗或用他克莫司或倍他米松治疗的FADS小鼠泪液中的骨膜蛋白。

结果

FADS小鼠表现出严重的睑缘炎和面部抓挠行为。在这些小鼠中,角膜上皮和基质显示增生,伴有嗜酸性粒细胞、肥大细胞和T2/T2细胞浸润。骨膜蛋白在病变中显著表达,泪液骨膜蛋白上调。倍他米松对严重角膜病变和泪液骨膜蛋白水平升高的抑制作用比他克莫司更强。

结论

FADS小鼠是一种新型的AKC小鼠模型,可用于检测抗AKC药物的治疗效果。

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