IL-38 has an anti-inflammatory action in psoriasis and its expression correlates with disease severity and therapeutic response to anti-IL-17A treatment.
Laura Mercurio,Martina Morelli,Claudia Scarponi,Elan Z. Eisenmesser,Nunzianna Doti,Gianluca Pagnanelli,Emanuela Gubinelli,Cinzia Mazzanti,Andrea Cavani,Menotti Ruvo,Charles A. Dinarello,Cristina Albanesi,Stefania Madonna +12 more
TL;DR: It is demonstrated that skin and circulating IL-38 levels are reduced in psoriatic patients and in other skin diseases characterized by neutrophilic infiltrate and that administration of recombinant full-length IL- 38 counteracts in vitro the biological processes induced by IL-36γ in human keratinocytes and endothelial cells and attenuates in vivo the severity of the psoriasiform phenotype induced by IMQ in mice.
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Abstract: IL-36 cytokines, a subgroup of IL-1 family, comprise IL-36α, IL-36β, and IL-36γ agonists, abundantly expressed in psoriatic skin, and IL-36RA and IL-38 antagonists. In psoriatic skin, IL-36 cytokines interfere with keratinocyte cornification programs and induce the release of antimicrobial peptides and chemokines active on neutrophils and Th17 lymphocytes. To date, the role of IL-38 antagonist in psoriasis remains to be defined. Here, we demonstrate that skin and circulating IL-38 levels are reduced in psoriatic patients and in other skin diseases characterized by neutrophilic infiltrate. In psoriasis, the balance of IL-36γ agonist/IL-38 antagonist serum levels is in favor of agonists and is closely associated with disease severity. Interestingly, IL-38 is upregulated by anti-IL-17A biological treatment and positively correlates with the therapeutic efficacy of secukinumab in psoriatic patients. The downregulation of IL-38 expression is strictly related to keratinocyte de-differentiation triggered by the inflammatory cytokines IL-36γ, IL-17, and IL-22. Finally, we demonstrate that administration of recombinant full-length IL-38 counteracts in vitro the biological processes induced by IL-36γ in human keratinocytes and endothelial cells and attenuates in vivo the severity of the psoriasiform phenotype induced by IMQ in mice. Such effects are achieved by restoring the physiological programs of keratinocyte proliferation and differentiation, and reducing the immune cell infiltrates.
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Citations
The IL-1 family of cytokines and receptors in rheumatic diseases.
TL;DR: The main functions of the IL-1 family are innate immune reactions and inflammation, rather than acquired immunity, which can occur in several rheumatic diseases.
317
The Significance of IL-36 Hyperactivation and IL-36R Targeting in Psoriasis.
Stefania Madonna,Giampiero Girolomoni,Charles A. Dinarello,Charles A. Dinarello,Cristina Albanesi +4 more
TL;DR: The pathogenic mechanisms leading to the altered balance of IL-36 agonists/antagonists and the significance of this dysregulation in psoriasis are discussed to provide a theoretical basis for the development of novel therapeutic strategies based on IL- 36 agonist/antagonist manipulation in psoriatic skin.
122
Anti-inflammatory mechanisms of the novel cytokine interleukin-38 in allergic asthma.
Xiaoyu Sun,Tianheng Hou,Edwin Cheung,Tiffany Nga-Teng Iu,Victor Wai-Hou Tam,Ida Miu-Ting Chu,Miranda Sin-Man Tsang,Paul K.S. Chan,Christopher Wai-Kei Lam,Chun-Kwok Wong +9 more
TL;DR: IL-38 administration suppressed airway hyperreactivity and asthma-related IL-4 and IL-5 expression in humanized mice and provided a basis for the development of a regulatory cytokine-based treatment for allergic asthma.
IL-38: A New Player in Inflammatory Autoimmune Disorders
Lihui Xie,Zhaohao Huang,He Li,Xiuxing Liu,Song Guo Zheng,Wenru Su +5 more
- 05 Aug 2019
TL;DR: Current data support that the IL-38/IL-36R and/or IL- 38/ IL-1RAPL1 axis primarily play an anti-inflammatory role in the development and resolution of inflammatory autoimmune diseases and indicate a possible therapeutic benefit ofIL-38 in these diseases.
98
Spatially and cell-type resolved quantitative proteomic atlas of healthy human skin.
Beatrice Dyring-Andersen,Marianne B. Løvendorf,Fabian Coscia,Alberto Santos,Line Bruun Pilgaard Møller,Ana R. Colaço,Lili Niu,Michael Bzorek,Sophia Doll,Jørgen Lock Andersen,Rachael A. Clark,Lone Skov,Marcel B. M. Teunissen,Matthias Mann,Matthias Mann +14 more
TL;DR: A spatially-resolved quantitative proteomic atlas of human skin is described, describing the quantitative distribution of structural proteins, known and previously undescribed proteins specific to cellular subsets and those with specialized immunological functions such as cytokines and chemokines.
References
Imiquimod-Induced Psoriasis-Like Skin Inflammation in Mice Is Mediated via the IL-23/IL-17 Axis
Leslie van der Fits,Sabine Mourits,Jane S. A. Voerman,Marius Kant,Louis Boon,Jon D. Laman,Ferry Cornelissen,Anne-Marie Mus,Edwin Florencia,Errol P. Prens,Erik Lubberts +10 more
TL;DR: The sole application of the innate TLR7/8 ligand IMQ rapidly induces a dermatitis closely resembling human psoriasis, critically dependent on the IL-23/IL-17 axis.
Interleukin-22, a T H 17 cytokine, mediates IL-23-induced dermal inflammation and acanthosis
Yan Zheng,Dimitry M. Danilenko,Patricia Valdez,Ian Kasman,Jeffrey Eastham-Anderson,Jianfeng Wu,Wenjun Ouyang +6 more
TL;DR: The results suggest that TH17 cells, through the production of both IL-22 and IL-17, might have essential functions in host defence and in the pathogenesis of autoimmune diseases such as psoriasis.
1.9K
Immunology of Psoriasis
TL;DR: The genetic background of psoriasis and its relationship to immune function, specifically genetic mutations, key PSORS loci, single nucleotide polymorphisms, and the skin transcriptome are discussed.
1.5K
Interleukin-36–Receptor Antagonist Deficiency and Generalized Pustular Psoriasis
Slaheddine Marrakchi,Philippe Guigue,Blair R. Renshaw,Anne Puel,Xue-Yuan Pei,Sylvie Fraitag,Jihen Zribi,Elodie Bal,Céline Cluzeau,Maya Chrabieh,Jennifer E. Towne,Jason Douangpanya,Christian Pons,Sourour Mansour,Valérie Serre,Hafedh Makni,Nadia Mahfoudh,Faiza Fakhfakh,Christine Bodemer,Josué Feingold,Smail Hadj-Rabia,Michel Favre,Emmanuelle Génin,Mourad Sahbatou,Arnold Munnich,Jean-Laurent Casanova,John E. Sims,Hamida Turki,Hervé Bachelez,Asma Smahi +29 more
TL;DR: Aberrant interleukin-36Ra structure and function lead to unregulated secretion of inflammatory cytokines and generalized pustular psoriasis.
939
Mutations in IL36RN/IL1F5 are associated with the severe episodic inflammatory skin disease known as generalized pustular psoriasis
Alexandros Onoufriadis,Michael A. Simpson,Andrew Pink,Paola Di Meglio,Catherine H. Smith,Venu Pullabhatla,Jo Knight,Sarah L. Spain,Frank O. Nestle,A. David Burden,Francesca Capon,Richard C. Trembath,Jonathan Barker +12 more
TL;DR: Findings suggest loss of function of IL36RN as the genetic basis of GPP and implicate innate immune dysregulation in this severe episodic inflammatory disease, thereby highlighting IL-1 signaling as a potential target for therapeutic intervention.
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