[Identification of Langerhans cells in dermatology].

Jasna Lipozencić, Suzana Ljubojević
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Abstract

This paper describes our own findings on the role of Langerhans' cells in dermatology and discusses literature data on their detection in seven different dermatoses. The skin is an integral part of immune system. During the past 30 years, increasing evidence has been accumulated that the skin contains cellular elements which are needed for the initiation and expression of immune response. Langerhans' cells (LCs) are dendritic cells originating in the bone marrow. They reside mainly within stratified squamous epithelia and constitute approximately 2-4% of epithelial cells. LCs are epidermal antigen presenting cells which play a crucial role in allergic contact hypersensitivity, viral diseases, graft versus host disease and elimination of neo-plastic cell clones. They express antigens conjugated with major histocompatibility complex (MHC) class II positive molecules on their surfaces for presentation to T-helper lymphocytes. LCs cannot be identified in routinely prepared histologic testing but can be visualised at the light microscope level by histochemical and immunologic techniques. Appropriate methods for the detection of Langerhans' cells in dermatology (also shown by our own experience) are histoenzymatic methods of adenosintriphosphatase (ATP-ase), acid phosphatase (AP), alpha-naphthylacetatesterase (ANAE and peroxidase-antiperoxidase immunohistochemistry method with polyclonal S-100 protein antibody (PAP). LCs are the only cells in normal skin with ATP-ase activity. Histoenzymatic methods used in patients with atopic dermatitis, vitiligo, mycosis fungoides, Behcet's disease, lichen ruber planus, psoriasis vulgaris, irritant dermatitis and allergic contact dermatitis demonstrated LSs in epidermis and dermis. ANAE and AP showed concordance and were suitable histochemical markers for LC distribution and macrophages in the dermis in mycosis fungoides, atopic dermatitis, psoriasis vulgaris, irritant chronic dermatitis and Bechet's disease. Our experience of the human skin showed a strong activity of calcium-activated adenosine triphosphatase in LCs. LCs in the guinea pig skin can be demonstrated by Mg++ and Ca++ activated adenosine triphosphatase, but a stronger activity of Ca++ activated adenosine triphosphatase in LCs after irritation. Ca++ ATP-ase as an indicator of energy-dependent pump is the reflection of intracellular calcium level, which is a significant factor for regulating the growth and metabolism of the cells. LCs are found as target cells during the efferent phase of contact allergic reaction. Immunohistochemical methods, define the role of LCs in dermatology more precisely and allow complete immunologic recognition within the epidermis.

[皮肤病学郎格汉斯细胞的鉴定]。
本文描述了我们在皮肤病学中朗格汉斯细胞的作用的发现,并讨论了在七种不同皮肤病中检测朗格汉斯细胞的文献数据。皮肤是免疫系统的重要组成部分。在过去的30年里,越来越多的证据表明,皮肤含有启动和表达免疫反应所需的细胞成分。朗格汉斯细胞(LCs)是起源于骨髓的树突状细胞。它们主要存在于层状鳞状上皮内,约占上皮细胞的2-4%。LCs是表皮抗原提呈细胞,在过敏性接触超敏反应、病毒性疾病、移植物抗宿主病和新塑性细胞克隆的消除中起着至关重要的作用。它们表达与主要组织相容性复合体(MHC) II类阳性分子结合的抗原,在其表面呈递给t辅助淋巴细胞。lc不能在常规准备的组织学测试中识别,但可以通过组织化学和免疫技术在光镜水平上可视化。皮肤病学中适合检测朗格汉斯细胞的方法有腺苷三磷酸酶(ATP-ase)、酸性磷酸酶(AP)、α -萘基乙酰酯酶(ANAE)的组织酶法和过氧化物酶-抗过氧化物酶免疫组织化学多克隆S-100蛋白抗体(PAP)。lc是正常皮肤中唯一具有atp酶活性的细胞。在特应性皮炎、白癜风、蕈样真菌病、白塞氏病、扁平橡胶苔藓、寻常型牛皮癣、刺激性皮炎和过敏性接触性皮炎患者中使用的组织酶方法显示表皮和真皮中存在LSs。ANAE和AP具有一致性,是蕈样真菌病、特应性皮炎、寻常型牛皮癣、刺激性慢性皮炎和Bechet病真皮中LC分布和巨噬细胞的合适组织化学标志物。我们对人类皮肤的研究表明,LCs中钙活化的腺苷三磷酸酶具有很强的活性。豚鼠皮肤的lccs可以通过Mg++和Ca++激活的腺苷三磷酸酶来表现,但刺激后lccs中Ca++激活的腺苷三磷酸酶活性更强。ca2 ++ atp酶作为能量依赖泵的指标,反映细胞内钙水平,是调节细胞生长和代谢的重要因素。LCs是接触性过敏反应传出期的靶细胞。免疫组织化学方法更精确地定义了lc在皮肤病学中的作用,并允许在表皮内进行完全的免疫识别。
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