Interleukin‐21 in autoimmune and inflammatory skin diseases

Mesas-Fernández, Alberto; Bodner, E; Hilke, Franz J.; Meier, Katharina; Ghoreschi, Kamran; Solimani, Farzan

doi:10.1002/eji.202250075

Cited by 19 publications

(14 citation statements)

References 165 publications

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“…Furthermore, resident memory T cells similar to Tfh mainly express IL-17 and IL-21. These results suggest that T-dependent immune responses and IL-21 are involved in pemphigus [ 34 ].…”

Section: Discussionmentioning

confidence: 99%

Cut-off values for IL-21 and IL-23 as biochemical markers for pemphigus vulgaris

Al-Hasnawi,

AL-Drobie

2023

JMedLife

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Pemphigus vulgaris (PV) is a potentially fatal mucocutaneous autoimmune disease characterized by severe skin lesions. Interleukin-21 (IL-21) and IL-23 have been linked to several autoimmune inflammatory diseases that may have a critical role in PV immunopathogenesis, including T-helper 17 (Th17) development. This study aimed to compare the serum levels of IL-21 and IL-23 in patients with PV and healthy controls. This case-control study included 90 participants (45 patients and 45 controls). Serum IL-21 and IL-23 were measured using the Sandwich-ELISA method provided by Sunlong Biotech, China. The findings revealed statistically significant results for IL-21 O.D. and Conc. (p=0.012*) and highly significant results for IL-23 O.D. and Conc. (p=0.000**). Furthermore, cut-off values were established for IL-21 (O.D.=0.071 pg/mL, Conc.=6.468 pg/mL) and IL-23 (O.D.=0.141 pg/mL, Conc.=6.745 pg/mL). These results indicate a potential association between PV and IL-21, IL-23, and the identified cut-off values. The particular roles of cytokines and how they can be utilized to treat PV require more investigation. To our knowledge, this was the first study to detect a cut-off point for IL-21 and IL-23 that may be used as novel and cost-effective biochemical markers for disease diagnosis.

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“…Furthermore, resident memory T cells similar to Tfh mainly express IL-17 and IL-21. These results suggest that T-dependent immune responses and IL-21 are involved in pemphigus [ 34 ].…”

Section: Discussionmentioning

confidence: 99%

Cut-off values for IL-21 and IL-23 as biochemical markers for pemphigus vulgaris

Al-Hasnawi,

AL-Drobie

2023

JMedLife

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“…Pathogenically, the crucial event in pemphigus is the formation of antibodies binding desmosomal proteins, leading to a loss of keratinocyte adhesion 23 . Formation of autoantibodies is supported by autoreactive, human leukocyte antigen (HLA)‐restricted T‐cells, which demonstrate a prevalently Th2 but also Th17‐oriented phenotype during active disease 24–26 . HLA DRB1*04: 02 and HLA‐DQB1*05: 03 increase risk of pemphigus.…”

Section: Pemphigusmentioning

confidence: 99%

“…23 Formation of autoantibodies is supported by autoreactive, human leukocyte antigen (HLA)-restricted T-cells, which demonstrate a prevalently Th2 but also Th17-oriented phenotype during active disease. [24][25][26] HLA DRB1*04: 02 and HLA-DQB1*05: 03 increase risk of pemphigus. Concordantly, these HLA types are more prevalent in geographical regions where pemphigus is more frequent.…”

Section: Pemphigusmentioning

confidence: 99%

Pemphigus and pemphigoids: Clinical presentation, diagnosis and therapy

Didona,

Schmidt,

Maglie

et al. 2023

J Deutsche Derma Gesell

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SummaryPemphigus and pemphigoid are two potentially life‐threatening groups of autoimmune diseases, characterized by autoantibodies targeting structural components of desmosomes or hemidesmosomes, respectively. Affected patients typically show itchy/painful plaques or blistering skin lesions and/or impairing mucosal blistering and erosions, which may strongly impact their quality of life. Since the milestone work of Walter Lever in 1953, who differentiated these two groups of diseases by histopathological analysis of the level of antibody‐mediated skin cleavage, enormous progresses occurred. Achievements made in laboratory diagnostics now allow to identify antigen specific structural proteins of the skin that are targeted by pathogenic autoantibodies. These progresses were accompanied by an increased understanding of the pathogenesis of these diseases thanks to the establishment of animal models reproducing disease and on studies on skin and blood of affected individuals, which have been leading to novel and disease‐specific treatments. Yet, given their phenotypical overlap with more common dermatological diseases, correct diagnosis and appropriate treatment are often delayed, in some cases leading to irreversible sequelae, including organ dysfunction (i.e., loss of vision in mucous membrane pemphigoid). Here, we provide a concise overview of the clinical appearance, diagnosis and therapeutic management of pemphigus and pemphigoid diseases.

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“…Pathogenetisch führt die Bindung von Antikörper an desmosomale Proteine zu einem Verlust der Keratinozytenadhäsion 23 . Die Bildung von Autoantikörpern wird durch autoreaktive, auf humane Leukozytenantigene (HLA) beschränkte T‐Zellen unterstützt, die während der aktiven Erkrankung einen überwiegend Th2‐, aber auch Th17‐orientierten Phänotyp aufweisen 24–26 . HLA DRB1*04: 02 und HLA‐DQB1*05:03 erhöhen das Risiko für Pemphigus.…”

Section: Pemphigusunclassified

“…23 Die Bildung von Autoantikörpern wird durch autoreaktive, auf humane Leukozytenantigene (HLA) beschränkte T-Zellen unterstützt, die während der aktiven Erkrankung einen überwiegend Th2-, aber auch Th17-orientierten Phänotyp aufweisen. [24][25][26] Pemphigus vulgaris (PV) ist durch zirkulierende IgG-Autoantikörper gegen Dsg3 und Dsg1 gekennzeichnet, die Akantholyse und suprabasale Blasenbildung an Haut und Schleimhäuten verursachen. 38 Das klinische Bild korreliert mit dem Antikörperprofil.…”

Section: Pemphigusunclassified

Pemphigus‐ und Pemphigoid‐Erkrankungen: Klinik, Diagnostik und Therapie

Didona,

Schmidt,

Maglie

et al. 2023

J Deutsche Derma Gesell

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ZusammenfassungPemphigus und Pemphigoid sind seltene Autoimmunkrankheiten der Haut mit potenziell lebensbedrohlichem Verlauf. Autoantikörper gegen epidermale und junktionale Strukturproteine (Desmosomen sowie Hemidesmosomen) führen bei Betroffenen typischerweise zu juckenden, schmerzhaften Plaques oder Blasen an der Haut und/oder Blasenbildung und Erosionen der Schleimhäute mit möglicher Einschränkung der Lebensqualität. Seit der bahnbrechenden Arbeit von Walter Lever im Jahr 1953, dem es gelang, mittels histopathologischer Untersuchung diese beiden Krankheitsgruppen anhand des Musters der Antikörper‐vermittelten Blasenbildung zu differenzieren, wurden enorme Fortschritte im Verständnis der Erkrankungen erzielt. Die Errungenschaften in der Labordiagnostik ermöglichten die Identifikation von Zielstrukturen zur präzisen Unterscheidung verschiedener Varianten der bullösen Autoimmunerkrankungen. Diese Fortschritte gingen dank der Entwicklung von Tiermodellen mit einem besseren Verständnis der Pathogenese einher. Außerdem haben Studien an Haut und Blut betroffener Patienten zu neuen und krankheitsspezifischen Behandlungen geführt. Aufgrund ihrer Seltenheit und der klinischen Ähnlichkeit mit anderen dermatologischen Erkrankungen verzögern sich die korrekte Diagnosestellung und die Einleitung einer entsprechenden Therapie häufig, was in einigen Fällen zu irreversiblen Folgeerscheinungen, einschließlich Funktionsstörungen von Organen (zum Beispiel Verlust des Sehvermögens beim Schleimhautpemphigoid) führt. Wir geben hier einen Überblick über das klinische Erscheinungsbild, den Diagnosealgorithmus und das therapeutische Management von Pemphigus‐ und Pemphigoid‐Erkrankungen.

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Interleukin‐21 in autoimmune and inflammatory skin diseases

Cited by 19 publications

References 165 publications

Cut-off values for IL-21 and IL-23 as biochemical markers for pemphigus vulgaris

Cut-off values for IL-21 and IL-23 as biochemical markers for pemphigus vulgaris

Pemphigus and pemphigoids: Clinical presentation, diagnosis and therapy

Pemphigus‐ und Pemphigoid‐Erkrankungen: Klinik, Diagnostik und Therapie

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