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银屑病的动物模型。

Animal models of psoriasis.

作者信息

Boehncke Wolf-Henning, Schön Michael P

机构信息

Department of Dermatology, University of Frankfurt, D-60590 Frankfurt, Germany.

出版信息

Clin Dermatol. 2007 Nov-Dec;25(6):596-605. doi: 10.1016/j.clindermatol.2007.08.014.

Abstract

Research into the pathogenesis of psoriasis has been severely hampered by the lack of a naturally occurring disorder in laboratory animals that mimics the complex phenotype and pathogenesis of the human disease. A large variety of spontaneous mutations, genetically engineered rodents, immunological reconstitution approaches, and xenotransplantation models have been used to study specific aspects of the pathophysiology of psoriasis, however. Several manipulations of resident cutaneous cell types or immigrating immunocytes appear to result in remarkably similar hyperproliferative inflammatory phenotypes in mice, thus suggesting that interfering with cutaneous homeostasis in general may ultimately result in a rather uniform reaction pattern that mirrors some features of psoriasis. Fully animal models of psoriasis have nonetheless not only shed light on the biological functions of given inflammatory mediators or other molecules but also tremendously contributed to the discussion on central pathogenic questions, such as the roles of innate and adaptive immune mechanisms, keratinocytes, and endothelial cells in psoriasis. Psoriasis research has also been greatly nourished by xenotransplantation of diseased or unaffected human skin onto immunocompromised recipients, an approach that has in many variations been used to study the role of T lymphocytes and other cells and that has been used for preclinical therapeutic studies. General approaches to generate animal models of psoriasis, features of some specific models, their value for psoriasis research, and their use for drug development are discussed in this article.

摘要

由于缺乏一种在实验动物中自然发生的、能模拟人类疾病复杂表型和发病机制的病症,银屑病发病机制的研究受到了严重阻碍。然而,人们已经使用了各种各样的自发突变、基因工程啮齿动物、免疫重建方法和异种移植模型来研究银屑病病理生理学的特定方面。对驻留皮肤细胞类型或迁移免疫细胞的几种操作似乎会在小鼠中导致非常相似的过度增殖性炎症表型,因此表明一般而言,干扰皮肤内环境稳态最终可能会导致一种相当一致的反应模式,这种模式反映了银屑病的一些特征。尽管如此,银屑病的完全动物模型不仅揭示了特定炎症介质或其他分子的生物学功能,还极大地促进了关于核心致病问题的讨论,例如先天性和适应性免疫机制、角质形成细胞和内皮细胞在银屑病中的作用。将患病或未患病的人类皮肤异种移植到免疫受损受体上也极大地推动了银屑病研究,这种方法有多种变体,已被用于研究T淋巴细胞和其他细胞的作用,并已用于临床前治疗研究。本文讨论了生成银屑病动物模型的一般方法、一些特定模型的特点、它们对银屑病研究的价值以及它们在药物开发中的应用。

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