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犬特应性皮炎不同临床方面的 IL-33 免疫表达。

Immunoexpression of IL-33 in the different clinical aspects of canine atopic dermatitis.

机构信息

Postgraduate Program in Animal Science, School of Medicine and Life Sciences, Pontifícia Universidade Católica do Paraná, Rua Imaculada Conceição 1155, Curitiba, PR 80215-901, Brazil.

Experimental Pathology Laboratory, School of Medicine and Life Sciences, Pontifícia Universidade Católica do Paraná, Rua Imaculada Conceição 1155, Curitiba, PR 80215-901, Brazil.

出版信息

Vet Immunol Immunopathol. 2024 Jul;273:110786. doi: 10.1016/j.vetimm.2024.110786. Epub 2024 May 26.

Abstract

Canine atopic dermatitis (CAD) is a chronic and inflammatory skin condition with a multifaceted origin, involving genetic factors, skin barrier abnormalities, immune responses, and hypersensitivity to various allergens. Interleukin 33 (IL-33), released by keratinocytes upon cellular injury, plays a crucial role in atopic dermatitis pathogenesis by inducing Th2 lymphocyte-mediated immune responses. This study aimed to evaluate IL-33 expression in dogs with atopic dermatitis and compare it to a control group. Forty-nine dogs were included, with 39 having atopic dermatitis, subdivided into groups based on clinical characteristics, and ten in the control group. Lesion and pruritus scores were assessed, and incisional biopsies were analyzed for dermatopathological characteristics. IL-33 expression was evaluated using immunohistochemistry, the analyses were blinded, based on the measurement of immunostaining areas using Image Pro-Plus software, version 4.5, relying on a semi-automatic color segmentation method, where the tissue immunostaining area for each biomarker was artificially delimited and quantified. Statistically significant differences in IL-33 immunostaining were found among groups (P=0.0005). Lichenified dogs (group 4) exhibited higher immunostaining compared to erythema (group 3) (P=0.0006), alesional pruritus (group 2) (P=0.0261), and the control group (group 1) (P=0.0079). IL-33 immunostaining increased with lesion progression, strongly correlating with lesion scores (P<0.0001), particularly in patients with chronic lesions characterized by erythema and lichenification. These findings suggest IL-33's significant role in canine atopic dermatitis pathogenesis and its association with lesion and inflammation scores during the chronic phase. This suggests potential therapeutic interventions targeting IL-33 or its receptors, though further studies are needed to explore these possibilities.

摘要

犬特应性皮炎(CAD)是一种慢性炎症性皮肤病,具有多方面的发病机制,涉及遗传因素、皮肤屏障异常、免疫反应和对各种过敏原的过敏反应。白细胞介素 33(IL-33)在角质形成细胞受到细胞损伤时释放,通过诱导 Th2 淋巴细胞介导的免疫反应,在特应性皮炎发病机制中发挥关键作用。本研究旨在评估犬特应性皮炎中 IL-33 的表达,并与对照组进行比较。共纳入 49 只犬,其中 39 只为特应性皮炎,根据临床特征分为几组,对照组为 10 只。评估病变和瘙痒评分,并对切口活检进行组织病理学特征分析。采用免疫组织化学法评估 IL-33 的表达,分析采用盲法,根据 Image Pro-Plus 软件版本 4.5 测量免疫染色面积,采用半自动颜色分割方法,对每个生物标志物的组织免疫染色面积进行人工划定和量化。发现各组之间的 IL-33 免疫染色存在统计学显著差异(P=0.0005)。苔藓样犬(第 4 组)的免疫染色强度高于红斑(第 3 组)(P=0.0006)、无病变瘙痒(第 2 组)(P=0.0261)和对照组(第 1 组)(P=0.0079)。IL-33 免疫染色随病变进展而增加,与病变评分强烈相关(P<0.0001),特别是在具有红斑和苔藓样变特征的慢性病变患者中。这些发现表明 IL-33 在犬特应性皮炎发病机制中具有重要作用,并且在慢性阶段与病变和炎症评分相关。这表明针对 IL-33 或其受体的潜在治疗干预可能是有必要的,但需要进一步研究来探索这些可能性。

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