在自身免疫性大疱性皮肤病的临床前模型中，靶向替代途径和C5而非C5a进行治疗可预防疾病发展。

Therapeutic targeting of alternative pathway and C5 but not C5a protects from disease development in a preclinical model of autoimmune blistering dermatosis.

作者信息

Laffer Björn, Ohms Mareike, Kenno Samyr, Tsui Ping, Ehlers-Jeske Elvira, Song Wenru, Song Wen-Chao, Köhl Jörg

机构信息

Institute for Systemic Inflammation Research, University of Lübeck, Lübeck, Germany.

Kira Pharmaceuticals, Research and Development, Cambridge, MA, United States.

出版信息

Front Immunol. 2025 Apr 30;16:1560468. doi: 10.3389/fimmu.2025.1560468. eCollection 2025.

DOI:10.3389/fimmu.2025.1560468

PMID:40370446

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12076022/

Abstract

INTRODUCTION

Epidermolysis Bullosa Acquisita (EBA) is an autoimmune blistering dermatosis characterized by autoantibodies (AAbs) against type VII collagen (COL7) located at the dermal epidermal junction (DEJ). Local complement activation drives C5a generation associated with neutrophil recruitment and activation resulting in skin lesions and inflammation. Here we tested the impact of C5a/C5adesArg, C5 or combined C5 and alternative pathway (AP) targeting on disease development and skin inflammation in a preclinical mouse model mimicking the effector phase of EBA.

METHODS

C57BL/6 mice were treated subcutaneously with purified rabbit anti-mouse-COL7 IgG in the presence of IgG1 mAbs directed against murine C5a/C5adesArg (M031), C5 (mBB5.1), a bifunctional protein comprising mBB5.1 fused to an active fragment of the AP inhibitor factor H (M014) or an IgG1 isotype control mAb. Formation of skin lesions was evaluated 12 days every other day. On day 12, DEJ separation, IgG AAb and C3b deposition and neutrophil infiltration was assessed.

RESULTS

Isotype IgG1-treated mice developed first skin lesions on day 4 peaking on day 12. Prophylactic treatment with either M031 or M014 markedly reduced the development of skin lesions, the dermal/epidermal separation and neutrophil recruitment. Surprisingly, C5 or combined AP/C5 inhibition by M014 but not C5a/C5adesArg-targeting by M031 reduced the development of skin lesions and dermal/epidermal separation in the setting of therapeutic treatment. IgG and C3b deposition was not affected by either treatment. Importantly, direct comparison of isolated C5 targeting by mBB5.1 vs. combined AP/C5 inhibition by M014 revealed that M014 reduced the development of skin lesions earlier and more pronounced than mBB5.1.

DISCUSSION

Our findings identify combined C5/AP targeting as a novel therapeutic option for autoimmune blistering dermatoses.

摘要

引言

获得性大疱性表皮松解症（EBA）是一种自身免疫性大疱性皮肤病，其特征是针对位于真皮表皮交界处（DEJ）的VII型胶原蛋白（COL7）产生自身抗体（AAbs）。局部补体激活驱动C5a生成，这与中性粒细胞募集和激活相关，从而导致皮肤病变和炎症。在此，我们在一个模拟EBA效应期的临床前小鼠模型中测试了C5a/C5adesArg、C5或C5与替代途径（AP）联合靶向对疾病发展和皮肤炎症的影响。

方法

在存在针对小鼠C5a/C5adesArg（M031）、C5（mBB5.1）、一种包含与AP抑制剂因子H的活性片段融合的mBB5.1的双功能蛋白（M014）或IgG1同种型对照单克隆抗体的情况下，将纯化的兔抗小鼠COL7 IgG皮下注射到C57BL/6小鼠体内。每隔一天评估12天皮肤病变的形成情况。在第12天，评估DEJ分离、IgG AAb和C3b沉积以及中性粒细胞浸润情况。

结果

同种型IgG1处理的小鼠在第4天出现首批皮肤病变，并在第12天达到峰值。用M031或M014进行预防性治疗可显著减少皮肤病变的发展、真皮/表皮分离和中性粒细胞募集。令人惊讶的是，M014对C5或联合AP/C5的抑制作用（而非M031对C5a/C5adesArg的靶向作用）在治疗性治疗中减少了皮肤病变的发展和真皮/表皮分离。IgG和C3b沉积不受任何一种治疗的影响。重要的是，对mBB5.1单独靶向C5与M014联合AP/C5抑制作用的直接比较显示，M014比mBB5.1更早且更显著地减少了皮肤病变的发展。