Detection of Type VII Collagen Autoantibodies Before the Onset of Bullous Systemic Lupus Erythematosus

Grabell, Daniel; Matthews, Loderick A.; Yancey, Kim B.; Chong, Benjamin F.

doi:10.1001/jamadermatol.2014.4409

Cited by 16 publications

(11 citation statements)

References 17 publications

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“…BSLE is caused by autoantibodies to the dermoepidermal junction, mainly the NC1 domain of type VII collagen, which is also a target antigen of epidermolysis bullosa acqusita (EBA). Anti‐type VII collagen autoantibodies can precede the clinical appearance of BSLE . IgG is found most frequently, followed by IgA and IgM.…”

Section: Discussionmentioning

confidence: 99%

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Recurrent oral ulcers and blisters in a young woman

et al. 2016

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Section: Discussionmentioning

confidence: 99%

“…Anti-type VII collagen autoantibodies can precede the clinical appearance of BSLE. 5 IgG is found most frequently, followed by IgA and IgM. Blisters are primarily present on sun-exposed areas, and show a predilection for the trunk, supraclavicular area, arms, face, vermillion border and oral mucosa.…”

Section: Discussionmentioning

confidence: 99%

Recurrent oral ulcers and blisters in a young woman

et al. 2016

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“…These anchoring fibrils mediate dermal–epidermal adhesion via binding of collagen VII to laminin-332 and collagen IV in the BM, and collagen I in the interstitial matrix [8]. Auto-antibodies against epitopes in the NC-1 domain cause the autoimmune skin blistering disorders epidermolysis bullosa acquisita (EBA) [85] and bullous systemic lupus erythematosus [86].…”

Section: Collagen VIImentioning

confidence: 99%

Basement membrane collagens and disease mechanisms

Gatseva

Sin

Brezzo

et al. 2019

Essays in Biochemistry

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Basement membranes (BMs) are specialised extracellular matrix (ECM) structures and collagens are a key component required for BM function. While collagen IV is the major BM collagen, collagens VI, VII, XV, XVII and XVIII are also present. Mutations in these collagens cause rare multi-systemic diseases but these collagens have also been associated with major common diseases including stroke. Developing treatments for these conditions will require a collective effort to increase our fundamental understanding of the biology of these collagens and the mechanisms by which mutations therein cause disease. Novel insights into pathomolecular disease mechanisms and cellular responses to these mutations has been exploited to develop proof-of-concept treatment strategies in animal models. Combined, these studies have also highlighted the complexity of the disease mechanisms and the need to obtain a more complete understanding of these mechanisms. The identification of pathomolecular mechanisms of collagen mutations shared between different disorders represent an attractive prospect for treatments that may be effective across phenotypically distinct disorders.

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“…Ein "u-serrated" Muster wird bei Bindung von AntiTyp VII Kollagen Antikörpern gefunden; dieses zeigt vermutlich den Verlauf der Ankerfibrillen von den Ankerplatten in die Lamina densa an bran verankert. Sie bilden daher einen wesentlichen funktionellen Mechanismus der dermoepidermalen Adhäsion [27,28]. Nur ganz selten werden beim bullösen SLE andere Autoantigene der Basalmembran als Zielstrukturen von zirkulierenden Autoantikörpern nachgewiesen, dazu zählen Laminin-332, Laminin-311 (früher als Laminin 6 bezeichnet) oder das bullöse Pemphigoidantigen II (BP-230-Antigen) [29].…”

Section: Diskussionunclassified