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红皮病活检组织的细胞因子谱分析揭示2型和17型免疫激活状态。

Cytokine Profiling of Erythroderma Biopsies Reveals Types 2 and 17 Immune Activation Status.

作者信息

Pukhalskaya Tatsiana, Finkelstein Mitchell, Miyake-Caballero Dacia A, Tetzlaff Michael T, North Jeffrey P, Cohen Jarish N

机构信息

Department of Dermatology and Pathology, University of California, California, USA.

Cooper Medical School of Rowan University, Camden, New Jersey, USA.

出版信息

J Cutan Pathol. 2025 Mar;52(3):235-243. doi: 10.1111/cup.14775. Epub 2024 Dec 12.

Abstract

BACKGROUND

Erythroderma is a dermatologic condition characterized by widespread red and scaly skin. The causes include, but are not limited to, psoriasis, eczema, drug eruptions, pityriasis rubra pilaris (PRP), and cutaneous T-cell lymphoma. Most of these are typified by Type 2 (e.g., eczema) or Type 17 (e.g., psoriasis) immune activation. However, since the clinicopathologic features of erythroderma can be nonspecific, assays that determine the underlying immune activation status are desirable.

METHODS

IL-13 RNA in situ hybridization and IL-36 immunohistochemistry were performed on 30 specimens of erythroderma, to ascertain Type 2 and Type 17 immune signatures, respectively.

RESULTS

Specimens of erythrodermic psoriasis and PRP showed strong expression of IL-36 and less than one IL-13-positive cell per millimeter. Conversely, those of spongiotic dermatitis showed low expression of IL-36 and greater than one IL-13-positive cell per millimeter. Most specimens of spongiotic, psoriasiform dermatitis demonstrated low IL-36 expression and greater than one IL-13-positive cell per millimeter, but a subset showed high IL-36 expression and greater than one IL-13-positive cell per millimeter.

CONCLUSIONS

We developed a Type 2/17 immune signature classifier based on cytokine profiling, which showed that cases of erythroderma fall within distinct categories of immune activation. This categorization may have utility in guiding clinical decisions.

摘要

背景

红皮病是一种以广泛的皮肤发红和脱屑为特征的皮肤病。其病因包括但不限于银屑病、湿疹、药物疹、红皮病型毛发红糠疹(PRP)和皮肤T细胞淋巴瘤。其中大多数以2型(如湿疹)或17型(如银屑病)免疫激活为典型特征。然而,由于红皮病的临床病理特征可能不具有特异性,因此需要能够确定潜在免疫激活状态的检测方法。

方法

对30例红皮病标本进行白细胞介素-13原位杂交和白细胞介素-36免疫组化,分别确定2型和17型免疫特征。

结果

红皮病型银屑病和PRP标本显示白细胞介素-36强表达,每毫米少于1个白细胞介素-13阳性细胞。相反,海绵状皮炎标本显示白细胞介素-36低表达,每毫米多于1个白细胞介素-13阳性细胞。大多数海绵状、银屑病样皮炎标本显示白细胞介素-36低表达,每毫米多于1个白细胞介素-13阳性细胞,但有一部分显示白细胞介素-36高表达,每毫米多于1个白细胞介素-13阳性细胞。

结论

我们基于细胞因子谱建立了一种2型/17型免疫特征分类器,结果表明红皮病病例属于不同类别的免疫激活。这种分类可能有助于指导临床决策。

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