Transglutaminases in autoimmune and inherited skin diseases: The phenomena of epitope spreading and functional compensation

Kárpáti, Sarolta; Sárdy, Miklós; Németh, Krisztián; Mayer, Balázs; Smyth, Neil; Paulsson, Mats; Traupe, Heiko

doi:10.1111/exd.13449

Cited by 50 publications

(44 citation statements)

References 108 publications

(160 reference statements)

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“…Histologically DH, such as other subepidermal autoimmune diseases, presents subepidermal blisters neutrophil and eosinophil infiltration and granular IgA deposition in the dermal papilla by DIF. DH patients show circulating IgA to TG3, which is the pivotal autoantigen ( 212 , 213 ). In most of DH patients, IgA to TG2 are detected, indicating an underlying, usually latent or mild celiac disease (CD) ( 212 , 213 ).…”

Section: Humoral Es In Autoimmune Bullous Diseasesmentioning

confidence: 99%

Humoral Epitope Spreading in Autoimmune Bullous Diseases

Didona

Zenzo

2018

Front. Immunol.

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Autoimmune blistering diseases are characterized by autoantibodies against structural adhesion proteins of the skin and mucous membranes. Extensive characterization of their autoantibody targets has improved understanding of pathogenesis and laid the basis for the study of antigens/epitopes diversification, a process termed epitope spreading (ES). In this review, we have reported and discussed ES phenomena in autoimmune bullous diseases and underlined their functional role in disease pathogenesis. A functional ES has been proposed: (1) in bullous pemphigoid patients and correlates with the initial phase of the disease, (2) in pemphigus vulgaris patients with mucosal involvement during the clinical transition to a mucocutaneous form, (3) in endemic pemphigus foliaceus, underlining its role in disease pathogenesis, and (4) in numerous cases of disease transition associated with an intermolecular diversification of immune response. All these findings could give useful information to better understand autoimmune disease pathogenesis and to design antigen/epitope specific therapeutic approaches.

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Section: Humoral Es In Autoimmune Bullous Diseasesmentioning

confidence: 99%

Humoral Epitope Spreading in Autoimmune Bullous Diseases

Didona

Zenzo

2018

Front. Immunol.

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“…TGs are Ca 2+ ‐dependent enzymes catalysing an irreversible crosslink of specific substrates forming a covalent isopeptide bond, in which a primary amine residue becomes attached to a glutamine acceptor . Three of the eight known TG isozymes are involved in formation of the CE: TG1, TG3 and TG5 crosslink proteins such as profilaggrin, involucrin, loricrin, trichohyalin and small proline‐rich proteins, representing constitutive components of the CE . TG1 specifically crosslinks sphingolipids, namely ceramides, to the protein envelope to achieve the linkage with the lipid envelope …”

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confidence: 99%

LEKTI domains D6, D7 and D8+9 serve as substrates for transglutaminase 1: implications for targeted therapy of Netherton syndrome

et al. 2019

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Background Transglutaminase (TG)1 plays a key role in the formation of the cornified envelope and thus in the maintenance of the epidermal barrier. Patients with Netherton syndrome (LEKTI deficiency) have increased activity of both TG1 and serin proteases. Objectives To determine whether there is a functional biochemical link between TG1 and LEKTI and whether LEKTI domains could possibly serve as substrates for TG1. Methods We analysed the protein sequence of LEKTI for possible TG1 recognition sites using bioinformatics. Synthetic peptides and recombinant LEKTI domains D6, D7 and D8+9 were examined in vitro and in situ for possible substrate specificity. The recombinant LEKTI domains were studied for inhibitory activity in a kallikrein (KLK)5 activity test. Results We identified possible TG1 consensus sequences in LEKTI domains D6, D7 and D8+9, pointing to a novel biological link between these two proteins. Indeed, synthesized short peptides from these consensus sequences were incorporated into the TG1 activity zone of the epidermis. In vitro the entire recombinant domains of LEKTI showed substrate specificity for TG1, which was again confirmed in situ. The inhibitory activity of the recombinant LEKTI domains was confirmed by a KLK5 inhibition test. The strongest inhibition was observed for domains D8+9. Conclusions There are specific domains of LEKTI that are recognized and processed by TG1. LEKTI domains D6, D7 and D8+9 contribute to the formation and protection of the cornified envelope. These results impact the development of protein replacement therapy approaches for Netherton syndrome.What's already known about this topic?• LEKTI and transglutaminase (TG)1 are key proteins involved in the terminal differentiation of the epidermis.• Lack of LEKTI causes Netherton syndrome; TG1 deficiency causes lamellar ichthyosis.• The serine protease inhibitor LEKTI is processed into different functional units. • Among different target proteases, kallikrein (KLK)5 appears to be a key player in disease pathology.• It has been demonstrated that LEKTI domain 6 inhibits KLK5 and KLK7; LEKTI domains 8-11 also inhibit KLK14.

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“…Epitope spreading has been reported to occur often during the first 3 months after a diagnosis of BP and is associated with disease severity (Di Zenzo et al, 2011). Epitope spreading has also been hypothesized to explain the onset of DH in patients with CD (Kárpáti et al, 2018). With regard to the present study, epitope spreading is a possible immunomechanism driving the association between DH and BP, but unfortunately, because this was a registry-based study, we had no access to the DIF findings or serum samples of the DH patients who developed BP subsequently and, therefore, we were unable to confirm or disprove this hypothesis.…”

Section: Discussionmentioning

confidence: 99%

Dermatitis Herpetiformis and Celiac Disease Increase the Risk of Bullous Pemphigoid

Varpuluoma

Jokelainen

Försti

et al. 2019

Journal of Investigative Dermatology

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Bullous pemphigoid (BP) and dermatitis herpetiformis (DH) are autoimmune bullous skin diseases. DH has been described to evolve into BP and the two diseases can have overlapping clinical appearances and diagnostic findings, but the association between DH and BP has not previously been studied in a large population. To evaluate DH and celiac disease as risk factors for BP, we conducted a retrospective case-control study of patients with BP and matched controls with basal cell carcinoma diagnosed in Finland between 1997 and 2013. A total of 3,397 patients with BP and 12,941 controls were included in the study. Forty-one (1.2%) BP patients and 7 (0.1%) controls had preceding DH. Diagnosed DH increased the risk of BP 22-fold (odds ratio ¼ 22.30; 95% confidence interval ¼ 9.99e49.70) and celiac disease 2-fold (odds ratio ¼ 2.54; 95% confidence interval ¼ 1.64e3.92) compared to controls. Eighteen (43.9%) of the patients who had DH and subsequent BP had bought dapsone during the 2 years prior to their BP diagnosis. Mean time between diagnosed DH and BP was 3 years. We conclude that diagnosis of DH is associated with a striking increase in the risk for BP.

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Transglutaminases in autoimmune and inherited skin diseases: The phenomena of epitope spreading and functional compensation

Cited by 50 publications

References 108 publications

Humoral Epitope Spreading in Autoimmune Bullous Diseases

Humoral Epitope Spreading in Autoimmune Bullous Diseases

LEKTI domains D6, D7 and D8+9 serve as substrates for transglutaminase 1: implications for targeted therapy of Netherton syndrome

Dermatitis Herpetiformis and Celiac Disease Increase the Risk of Bullous Pemphigoid

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