Abstract

Pemphigus vulgaris (PV) is a potentially life-threatening autoimmune blistering disease which is associated with autoantibodies directed against two desmosomal proteins, desmoglein (Dsg) 3 and 1. Treatment of PV is rather challenging and relies on the long-term use of systemic corticosteroids and additional immunosuppressants. More recently, autoantibody-depleting therapies such as rituximab, high-dose intravenous immunoglobulins, and immunoadsorption were shown to be valuable treatment options in PV. Specific removal of pathogenic autoantibodies would further increase efficacy and usability of immunoadsorption. Here, we tested the capacity of our recently developed prototypic Dsg1- and Dsg3-specific adsorbers to remove circulating pathogenic autoantibodies from three different PV patients. The pathogenic potential of the Dsg3/1-depleted IgG fractions and the anti-Dsg3-specific IgG was explored in two different in vitro assays based on cultured human keratinocytes, the desmosome degradation assay and the dispase-based dissociation assay. In addition, the neonatal mouse model of PV was used. In both in vitro assays, no difference between the pathogenic effect of total PV IgG and anti-Dsg3-specific IgG was seen, while Dsg3/1-depleted and control IgG were not pathogenic. For the samples of all 3 PV patients, depletion of anti-Dsg3/1 IgG resulted in a complete loss of pathogenicity when injected into neonatal mice. In contrast, injection of anti-Dsg3-specific IgG, eluted from the column, induced gross blistering in the mice. Our data clearly show that anti-Dsg3-specific IgG alone is pathogenic in vitro and in vivo, whereas Dsg3/1-depletion results in a complete loss of pathogenicity. Furthermore, our data suggest that Dsg-specific adsorption may be a suitable therapeutic modality to efficiently reduce pathogenic autoantibodies in patients with severe PV.

Highlights

  • Pemphigus vulgaris (PV) is a potentially life-threatening intraepidermal blistering autoimmune disease [1,2,3,4]

  • In PV patients with exclusive mucosal involvement, autoantibodies are restricted to Desmoglein 3 (Dsg3), whereas autoantibodies against both Dsg3 and desmoglein 1 (Dsg1) are associated with skin and mucosal lesions [10,11,12]

  • To study the effect of Dsg-specific normal human immunoglobulin G (IgG) we focused on anti-Dsg3-specific IgG since only two of the three PV patients revealed Dsg1specifc IgG

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Summary

Introduction

Pemphigus vulgaris (PV) is a potentially life-threatening intraepidermal blistering autoimmune disease [1,2,3,4]. Desmoglein 3 (Dsg3) and desmoglein 1 (Dsg1) have been identified as autoantigens in PV [5,6,7,8]. Dsg and Dsg are desmosomal transmembrane cadherins that mediate intercellular adhesion of keratinocytes in the skin and surface-close epithelia [3, 6, 9]. In PV patients with exclusive mucosal involvement (mPV), autoantibodies are restricted to Dsg, whereas autoantibodies against both Dsg and Dsg are associated with skin and mucosal lesions (mucocutaneous type of PV, mcPV) [10,11,12]. In pemphigus foliaceus (PF), autoantibody reactivity is limited to Dsg and patients only develop skin lesions. Albeit not undisputed, evidence for the pathogenic effect of anti-Dsg1/3 antibodies has been provided, less data were reported about the pathogenicity of non-Dsg antibodies [13, 15,16,17,18,19,20]

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