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Recent advances in the study of the pathophysiology of pemphigus.

机译:天疱疮的病理生理研究的最新进展。

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Recent rapid advances in the basic research into pemphigus have provided many insights into its pathophysiology. In particular, a recently developed enzyme-linked immunosorbent assay (ELISA) for desmogleins 1 and 3 (Dsg1 and Dsg3), antigens for pemphigus foliaceus (PF) and pemphigus vulgaris (PV), respectively, has led to great progress in the diagnosis and classification of pemphigus, as well as in understanding its pathomechanisms. Studies with the anti-Dsg1 and anti-Dsg3 antibodies have indicated that there are two types of PV, the mucosal dominant type and the mucocutaneous type. The same ELISA has identified the antigens in pemphigus herpetiformis. The autoantigens detected by this ELISA correlate well with the clinical features in pemphigus patients in showing the shift between PV and PF. In addition, the Dsg compensation theory proposed by Stanley and Amagai can reasonably explain the different depths of skin lesions and the different occurrences of skin and oral mucosal lesions between PV and PF. Furthermore, a complicated profile of autoantigens in paraneoplastic pemphigus (PNP) has been indicated in various biochemical studies, and IgG anti-Dsg1 and anti-Dsg3 antibodies have been detected in serum from all the PNP patients by the above ELISA. On the other hand, serum from subcorneal pustular dermatosis type IgA pemphigus patients have been shown to react with Dsc1, another type of desmosomal cadherin, by a novel cDNA transfection method. In addition, IgA anti-Dsg1 and anti-Dsg3 antibodies have been detected in a few patients with IgA pemphigus by an ELISA for IgA antibodies. Various autoimmune bullous diseases, including several types of pemphigus, are the only diseases in which the pathogenic role of circulating autoantibodies has been confirmed using the newborn mouse animal model. Therefore, studies of the pathophysiology of pemphigus are extremely important as a paradigm for research into various types of autoimmune diseases in other fields.
机译:天疱疮基础研究的最新快速进展为其病理生理学提供了许多见识。特别是,最近开发的用于桥粒糖蛋白1和3(Dsg1和Dsg3),叶蝇天疱疮(PF)和寻常性天疱疮(PV)的抗原的酶联免疫吸附测定(ELISA)在诊断和诊断方面取得了长足的进步。天疱疮的分类,以及了解天疱疮的发病机理。对抗Dsg1和抗Dsg3抗体的研究表明,PV有两种类型,即粘膜优势型和粘膜皮肤型。相同的ELISA已鉴定出天疱疮的抗原。通过ELISA检测到的自身抗原与天疱疮患者的临床特征密切相关,显示了PV和PF之间的变化。此外,Stanley和Amagai提出的Dsg补偿理论可以合理地解释PV和PF之间皮肤病变深度的不同以及皮肤和口腔粘膜病变的发生率。此外,在各种生化研究中已表明副肿瘤性天疱疮(PNP)中自身抗原的复杂情况,并且通过上述ELISA在所有PNP患者的血清中均检测到IgG抗Dsg1和抗Dsg3抗体。另一方面,已显示出通过新颖的cDNA转染方法,来自角膜下脓疱性皮肤病IgA型天疱疮患者的血清与另一种桥粒钙粘蛋白Dsc1反应。另外,已经通过IgA抗体的ELISA在少数IgA天疱疮患者中检测到IgA抗Dsg1和抗Dsg3抗体。多种自身免疫性大疱性疾病,包括几种类型的天疱疮,是唯一可以通过新生小鼠动物模型证实的循环自身抗体的致病作用的疾病。因此,天疱疮的病理生理学研究作为在其他领域研究各种类型的自身免疫性疾病的范例非常重要。

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