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天疱疮治疗的新方法。

New approaches to the treatment of pemphigus.

作者信息

Grando Sergei A

机构信息

Department of Dermatology, University of California, Davis, California, USA.

出版信息

J Investig Dermatol Symp Proc. 2004 Jan;9(1):84-91. doi: 10.1111/j.1087-0024.2004.00826.x.

DOI:10.1111/j.1087-0024.2004.00826.x
PMID:14870992
Abstract

In pemphigus vulgaris, treatment with systemic glucocorticosteroids is life saving; it may, however, cause severe side effects, including death. A patient with pemphigus vulgaris and myasthenia gravis was treated for approximately five years with the cholinomimetic Mestinon (pyridostigmine bromide), Imuran (azathioprine), and a topical corticosteroid gel before the need to introduce systemic glucocorticosteroids. Because activation of keratinocyte acetylcholine receptors also has been shown to abolish pemphigus IgG-induced acantholysis in cultured keratinocyte monolayers, a clinical trial of Mestinon was initiated in patients with active pemphigus vulgaris, pemphigus foliaceus, and paraneoplastic autoimmune multiorgan syndrome (also known as paraneoplastic pemphigus). First results indicate that nonsteroidal treatment of pemphigus is possible. Mestinon may be used to slow down progression of the disease and to treat mild cases with chronic lesions on limited areas. Stimulation of the keratinocyte- acetylcholine axis may lead to a therapeutic effect through any of the following mechanisms: (1) stimulating keratinocyte cell-to-cell attachment; (2) accelerating reepithelialization; and (3) competing with the disease-causing pemphigus antibodies, preventing them from attachment to keratinocytes. Glucocorticosteroids and various types of steroid-sparing drugs used to treat pemphigus exhibit cholinergic side effects, including effects on expression and function of keratinocyte adhesion molecules, that are very similar to those produced by the cholinomimetic drugs. Further elucidation of the mechanisms underlying therapeutic efficacy of antiacantholytics may shed light on the immunopharmacological mechanisms of pemphigus antibody-induced acantholysis.

摘要

在寻常型天疱疮中,全身应用糖皮质激素治疗可挽救生命;然而,它可能会引起严重的副作用,包括死亡。一名患有寻常型天疱疮和重症肌无力的患者在需要引入全身糖皮质激素之前,用拟胆碱药美斯的明(溴吡斯的明)、硫唑嘌呤和一种外用糖皮质激素凝胶治疗了约五年。由于在培养的角质形成细胞单层中,角质形成细胞乙酰胆碱受体的激活也已被证明可消除天疱疮IgG诱导的棘层松解,因此对活动性寻常型天疱疮、落叶型天疱疮和副肿瘤性自身免疫性多器官综合征(也称为副肿瘤性天疱疮)患者启动了美斯的明的临床试验。初步结果表明,天疱疮的非甾体治疗是可能的。美斯的明可用于减缓疾病进展,并治疗有限区域有慢性病变的轻症病例。刺激角质形成细胞 - 乙酰胆碱轴可能通过以下任何一种机制产生治疗效果:(1)刺激角质形成细胞间的细胞黏附;(2)加速上皮再形成;(3)与致病的天疱疮抗体竞争,防止它们附着于角质形成细胞。用于治疗天疱疮的糖皮质激素和各种类型的糖皮质激素节省药物表现出胆碱能副作用,包括对角质形成细胞黏附分子表达和功能的影响,这些副作用与拟胆碱药产生的副作用非常相似。对抗棘层松解剂治疗效果的潜在机制的进一步阐明可能会揭示天疱疮抗体诱导棘层松解的免疫药理学机制。

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