Cross-reactivity of autoantibodies from patients with epidermolysis bullosa acquisita with murine collagen VII

Csorba, Kinga; Sesărman, Alina; Oswald, Eva; Feldrihan, Vasile; Fritsch, Anja; Hashimoto, Takashi; Sitaru, Cassian

doi:10.1007/s00018-009-0256-3

Cited by 21 publications

(33 citation statements)

References 32 publications

(64 reference statements)

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“…We further showed that all antibodies generated here, which were directed to different epitopes of human COL7 NC1, led to dermal-epidermal separation ex vivo, as reported previously using other fragments of COL7 (Csorba et al, 2010). Split formation was dependent on the presence of neutrophils, whereas incubation of human skin with antibodies alone did not cause pathology.…”

Section: Discussionsupporting

confidence: 83%

Autoantibodies to Multiple Epitopes on the Non-Collagenous-1 Domain of Type VII Collagen Induce Blisters

Vorobyev

Ujiie

Recke

et al. 2015

Journal of Investigative Dermatology

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Epidermolysis bullosa acquisita (EBA) is an autoimmune blistering disease of the skin and mucous membranes, characterized by autoantibodies against type VII collagen (COL7), a major component of anchoring fibrils. Different clinical EBA phenotypes are described, including mechanobullous and inflammatory variants. Most EBA patients' sera react with epitopes located within the non-collagenous 1 (NC1) domain of human COL7. However, it has remained unclear whether antibody binding to these different epitopes is pathogenically relevant. To address this issue, we generated recombinant proteins covering the entire NC1 domain. IgG reactivity with these proteins was analyzed in sera of 69 EBA patients. Most recognized clusters of epitopes throughout the NC1 domain. No correlation was detected between antibody specificity and clinical phenotype. To study the pathogenicity of antibodies specific to different NC1 subdomains, rabbit antibodies were generated. All these antibodies caused dermal-epidermal separation ex vivo. Antibodies against two of these subdomains were injected into mice carrying null mutations of mouse COL7 and the human COL7 transgene and induced subepidermal blisters. We here document that autoantibodies to COL7, independent of the targeted epitopes, induce blisters both ex vivo and in vivo. In addition, using COL7-humanized mice, we provide in vivo evidence of pathogenicity of autoantibodies binding to human COL7.

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Section: Discussionsupporting

confidence: 83%

Autoantibodies to Multiple Epitopes on the Non-Collagenous-1 Domain of Type VII Collagen Induce Blisters

Vorobyev

Ujiie

Recke

et al. 2015

Journal of Investigative Dermatology

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“…The recombinant fragments designated GST-mCXVII-EC1, GST-mCXVII-EC3, GST-mCXVII-EC7 and GST-mCXVII-IC2 contain murine collagen XVII sequences stretching from amino acid positions 498–580, 856–901, 1030–1134, and 186–475, respectively [31]. These GST-fusion proteins containing sequences of murine BP180/CXVII were cloned and purified as previously described [31], [41]. Briefly, recombinant GST fusion and His-tagged proteins were expressed in E. coli TOP10 and XL1-Blue and purified by gluthatione agarose and metallochelate affinity chromatography, respectively as described [16], [42].…”

Section: Methodsmentioning

confidence: 99%

“…Six-micrometer cryosections of murine or human skin were washed in PBS to remove embedding medium and incubated with 100 µl of diluted antibody preparations for 2–3 h at 37°C. Sections were washed twice with PBS and chambers were prepared as previously described [41]. Human leukocytes were isolated from the peripheral blood of healthy donors.…”

Section: Methodsmentioning

confidence: 99%

The Flavonoid Luteolin Inhibits Fcγ-Dependent Respiratory Burst in Granulocytes, but Not Skin Blistering in a New Model of Pemphigoid in Adult Mice

et al. 2012

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Bullous pemphigoid is an autoimmune blistering skin disease associated with autoantibodies against the dermal-epidermal junction. Passive transfer of antibodies against BP180/collagen (C) XVII, a major hemidesmosomal pemphigoid antigen, into neonatal mice results in dermal-epidermal separation upon applying gentle pressure to their skin, but not in spontaneous skin blistering. In addition, this neonatal mouse model precludes treatment and observation of diseased animals beyond 2–3 days. Therefore, in the present study we have developed a new disease model in mice reproducing the spontaneous blistering and the chronic course characteristic of the human condition. Adult mice were pre-immunized with rabbit IgG followed by injection of BP180/CXVII rabbit IgG. Mice pre-immunized against rabbit IgG and injected 6 times every second day with the BP180/CXVII-specific antibodies (n = 35) developed spontaneous sustained blistering of the skin, while mice pre-immunized and then treated with normal rabbit IgG (n = 5) did not. Blistering was associated with IgG and complement C3 deposits at the epidermal basement membrane and recruitment of inflammatory cells, and was partly dependent on Ly-6G-positive cells. We further used this new experimental model to investigate the therapeutic potential of luteolin, a plant flavonoid with potent anti-inflammatory and anti-oxidative properties and good safety profile, in experimental BP. Luteolin inhibited the Fcγ-dependent respiratory burst in immune complex-stimulated granulocytes and the autoantibody-induced dermal-epidermal separation in skin cryosections, but was not effective in suppressing the skin blistering in vivo. These studies establish a robust animal model that will be a useful tool for dissecting the mechanisms of blister formation and will facilitate the development of more effective therapeutic strategies for managing pemphigoid diseases.

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“…Rabbit immune complexes were formed using a recombinant form of mouse collagen VIIC (GST-mCVIICr) and sera from a rabbit immunized against this protein [21]. Briefly, 96-well microtiter plates were coated with 5 g of GST-hCXVII-NC16A or 5 g of GST-mCVIICr in 0.1 M bicarbonate buffer (pH 9.6).…”

Section: Ros Measurement By Luminol Chemiluminescencementioning

confidence: 99%

“…The ability of BP patients' autoantibodies to activate human and murine leukocytes was assessed using an ex vivo assay of antibodyinduced granulocyte-dependent dermal-epidermal separation in cryosections of normal human skin, as described previously [21,22].…”

Section: Ex Vivo Cryosection Assaymentioning

confidence: 99%

Why human pemphigoid autoantibodies do not trigger disease by the passive transfer into mice?

Sesărman¹,

Oswald²,

Chiriac³

et al. 2012

Immunology Letters

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Cross-reactivity of autoantibodies from patients with epidermolysis bullosa acquisita with murine collagen VII

Cited by 21 publications

References 32 publications

Autoantibodies to Multiple Epitopes on the Non-Collagenous-1 Domain of Type VII Collagen Induce Blisters

Autoantibodies to Multiple Epitopes on the Non-Collagenous-1 Domain of Type VII Collagen Induce Blisters

The Flavonoid Luteolin Inhibits Fcγ-Dependent Respiratory Burst in Granulocytes, but Not Skin Blistering in a New Model of Pemphigoid in Adult Mice

Why human pemphigoid autoantibodies do not trigger disease by the passive transfer into mice?

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