寻常型银屑病中角桥粒芯蛋白的表达不同于正常皮肤和其他炎症性皮肤病。

Corneodesmosin expression in psoriasis vulgaris differs from normal skin and other inflammatory skin disorders.

作者信息

Allen M, Ishida-Yamamoto A, McGrath J, Davison S, Iizuka H, Simon M, Guerrin M, Hayday A, Vaughan R, Serre G, Trembath R, Barker J

机构信息

St. John's Institute of Dermatology, King's College, London, University of Leicester, Leicester, United Kingdom.

出版信息

Lab Invest. 2001 Jul;81(7):969-76. doi: 10.1038/labinvest.3780309.

DOI:10.1038/labinvest.3780309

PMID:11454986

Abstract

Corneodesmosin (Cdsn) is a late differentiation epidermal glycoprotein putatively involved in keratinocyte adhesion. The Cdsn gene lies within the susceptibility region on chromosome 6p21.3 (PSORS1) for psoriasis, a common chronic disfiguring skin disease. A particular allelic variant of Cdsn has a strong association with psoriasis. Therefore, genetically and biologically, Cdsn is a possible candidate gene for psoriasis susceptibility. To investigate a potential role for Cdsn in psoriasis pathogenesis, protein expression studies were performed by quantitative immunohistochemistry on normal skin, psoriatic skin (lesional and nonlesional), and other skin disorders using monoclonal antibodies (G36-19 and F28-27). In normal and nonlesional skin, Cdsn was expressed in stratum corneum and one or two layers of superficial stratum granulosum. In lesional psoriasis, there was a significant increase in Cdsn expression, which was observed in multiple layers of stratum spinosum and in stratum corneum. The expression pattern varied from granular, cytoplasmic immunoreactivity to cell surface labeling with weakly immunoreactive cytoplasm. In chronic atopic dermatitis, lichen planus, mycosis fungoides, and pityriasis rubra pilaris, Cdsn immunoreactivity was confined to stratum corneum and upper stratum granulosum with no stratum spinosum immunoreactivity. Immunoelectron microscopy of normal and lesional psoriatic skin demonstrated Cdsn release concomitant with involucrin incorporation into cell envelopes and completed before mature envelope formation. Extracellular release of Cdsn occurred at a lower level of the epidermis in psoriasis than normal skin. These protein expression studies provide evidence of altered Cdsn expression in psoriasis consistent with a role of Cdsn in disease pathogenesis. Further functional and genetic studies of Cdsn are justified to determine its role as a potential psoriasis-susceptibility factor.

摘要

角质桥粒芯蛋白（Cdsn）是一种晚期分化的表皮糖蛋白，可能参与角质形成细胞的黏附。Cdsn基因位于6号染色体p21.3（PSORS1）上的银屑病易感区域，银屑病是一种常见的慢性毁容性皮肤病。Cdsn的一种特定等位基因变体与银屑病密切相关。因此，从遗传学和生物学角度来看，Cdsn是银屑病易感性的一个可能候选基因。为了研究Cdsn在银屑病发病机制中的潜在作用，我们使用单克隆抗体（G36 - 19和F28 - 27），通过定量免疫组织化学对正常皮肤、银屑病皮肤（皮损和非皮损）以及其他皮肤疾病进行了蛋白质表达研究。在正常和非皮损皮肤中，Cdsn表达于角质层和一到两层浅表颗粒层。在银屑病皮损中，Cdsn表达显著增加，在棘层多层细胞和角质层中均可观察到。其表达模式从颗粒状、细胞质免疫反应性到细胞表面标记且细胞质免疫反应性较弱不等。在慢性特应性皮炎、扁平苔藓、蕈样肉芽肿和毛发红糠疹中，Cdsn免疫反应性局限于角质层和上层颗粒层，棘层无免疫反应性。正常和银屑病皮损皮肤的免疫电子显微镜检查显示，Cdsn的释放与内披蛋白掺入细胞包膜同时发生，并在成熟包膜形成之前完成。银屑病中Cdsn的细胞外释放发生在表皮比正常皮肤更低的水平。这些蛋白质表达研究提供了证据，表明银屑病中Cdsn表达改变，这与Cdsn在疾病发病机制中的作用一致。对Cdsn进行进一步的功能和遗传学研究是合理的，以确定其作为潜在银屑病易感因素的作用。