Lübeck Institute of Experimental Dermatology, University of Lübeck, Lübeck, Germany.
Institute of Virology and Cell Biology, University of Lübeck, Lübeck, Germany.
Front Immunol. 2022 Feb 7;12:812627. doi: 10.3389/fimmu.2021.812627. eCollection 2021.
Mucous membrane pemphigoid (MMP) is an autoimmune blistering disease characterized by autoantibodies against the basal membrane zone of skin and surface-close epithelia and predominant mucosal lesions. The oral cavity and conjunctivae are most frequently affected, albeit clinical manifestations can also occur on the skin. MMP-associated lesions outside the oral cavity typically lead to scarring. Mechanisms underlying scarring are largely unknown in MMP and effective treatment options are limited. Herein, we assessed the collagen architecture in tissue samples of an antibody-transfer mouse model of anti-laminin-332 MMP. In MMP mice, increased collagen fibril density was observed in skin and conjunctival lesions compared to mice injected with normal rabbit IgG. The extracellular matrix of MMP skin samples also showed altered post-translational collagen cross-linking with increased levels of both lysine- and hydroxylysine-derived collagen crosslinks supporting the fibrotic phenotype in experimental MMP compared to control animals. In addition, we evaluated a potential anti-fibrotic therapy in experimental anti-laminin-332 MMP using disulfiram, an inhibitor of the aldehyde dehydrogenase (ALDH), which has been implicated in immune-mediated mucosal scarring. In addition, disulfiram also acts as a copper chelator that was shown to block lysyl oxidase activity, an enzyme involved in formation of collagen crosslinks. Topical use of disulfiram (300 μM in 2% [w/v] methocel) did not improve ocular lesions in experimental MMP over the 12-day treatment period in disulfiram-treated mice compared to vehicle-treated mice (n=8/group). Furthermore, C57BL6/J mice (n=8/group) were treated prophylactically with 200 mg/kg p.o. disulfiram or the solvent once daily over a period of 12 days. Systemic treatment did not show any reduction in the severity of oral and ocular lesions in MMP mice, albeit some improvement in skin lesions was observed in disulfiram- vs. vehicle-treated mice (p=0.052). No reduction in fibrosis was seen, as assessed by immunohistochemistry. Whilst blocking of ALDH failed to significantly ameliorate disease activity, our data provide new insight into fibrotic processes highlighting changes in the collagenous matrix and cross-linking patterns in IgG-mediated MMP.
黏膜性类天疱疮(Mucous membrane pemphigoid,MMP)是一种自身免疫性水疱性疾病,其特征为皮肤和黏膜上皮基底膜带自身抗体,并以黏膜损害为主。口腔和结膜最常受累,尽管皮肤也可出现临床表现。口腔外的 MMP 相关病变通常导致瘢痕形成。MMP 中瘢痕形成的机制在很大程度上尚不清楚,有效的治疗选择有限。在此,我们评估了抗层粘连蛋白 332 MMP 抗体转移小鼠模型组织样本中的胶原结构。与注射正常兔 IgG 的小鼠相比,MMP 小鼠的皮肤和结膜病变中胶原纤维密度增加。MMP 皮肤样本的细胞外基质也表现出翻译后胶原交联的改变,赖氨酸和羟赖氨酸衍生的胶原交联水平升高,支持实验性 MMP 中的纤维化表型与对照动物相比。此外,我们评估了使用二硫化四乙基秋兰姆(disulfiram)治疗实验性抗层粘连蛋白 332 MMP 的潜在抗纤维化治疗方法,二硫化四乙基秋兰姆是一种醛脱氢酶(aldehyde dehydrogenase,ALDH)抑制剂,与免疫介导的黏膜瘢痕形成有关。此外,二硫化四乙基秋兰姆还作为铜螯合剂发挥作用,可阻断赖氨酰氧化酶活性,该酶参与胶原交联的形成。与 vehicle 治疗的小鼠相比,在二硫化四乙基秋兰姆治疗的小鼠中,眼部病变在 12 天的治疗期间未得到改善(n=8/组)。此外,C57BL6/J 小鼠(n=8/组)每天预防性口服 200mg/kg 二硫化四乙基秋兰姆或溶剂 12 天。系统治疗并未显示 MMP 小鼠口腔和眼部病变严重程度的任何降低,尽管二硫化四乙基秋兰姆治疗的小鼠皮肤病变有所改善(p=0.052)。免疫组化显示纤维化无减少。尽管阻断 ALDH 未能显著改善疾病活动度,但我们的数据为纤维化过程提供了新的见解,强调了 IgG 介导的 MMP 中胶原基质和交联模式的变化。
