Interleukin-31: A Pro-inflammatory Oriented Cytokine

Giuseppe Murdaca; Francesca Paladin; Andrea Orsi; Sebastiano Gangemi

doi:10.31083/FBL37462

Frontiers in Bioscience-Landmark ›› 2025, Vol. 30 ›› Issue (6) :37462 DOI: 10.31083/FBL37462

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Interleukin-31: A Pro-inflammatory Oriented Cytokine

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Abstract

Type 2 immunity is represented by T helper 2 (Th2) lymphocytes and the cytokines produced downstream (Interleukin (IL)-4, IL-13, IL-31). They are increasingly recognized as pivotal mediators in the pathogenesis of immune-mediated dermatological conditions such as atopic dermatitis (AD) and psoriasis (Pso). In these disorders, they initiate and amplify immunological signaling cascades, promote cutaneous inflammation, and contribute to the induction of pruritus. In this context, IL-33 and IL-31 would be believed to be intrinsically linked and related to the acuity of the disease. The presence of an interleukin could in fact trigger the other, amplifying the inflammatory process of itchy skin disorders and therefore the extent of the symptoms. High levels of IL-31 may support the maintenance of a microenvironment that promotes both the growth and spread of solid tumors, as well as the development of cancer-associated pruritus. Given these premises, non-histaminergic mediators such as IL-31 and IL-33 could be explored as novel therapeutic targets for the treatment of pruritus in immune-mediated skin diseases and cancer, improving the QoL of patients. Finally, we briefly discussed the recent innovations in the field of monoclonal anti-IL-31 therapies.

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IL-31 / IL-33 / IL-33/IL-31 axis / IL-31 receptors / cancer

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Giuseppe Murdaca, Francesca Paladin, Andrea Orsi, Sebastiano Gangemi. Interleukin-31: A Pro-inflammatory Oriented Cytokine. Frontiers in Bioscience-Landmark, 2025, 30(6): 37462 DOI:10.31083/FBL37462

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1. Introduction

Interleukin 31 (IL-31) belongs to the IL-6 superfamily, which includes among others IL-11, IL-21, IL-27, oncostatin M (OSM), leukemia inhibitory factor, and cardiotropin 1 [1]. This cytokine is mainly produced by type II helper (Th2) lymphocytes, monocytes/macrophages, mast cells, basophils, dendritic cells, fibroblasts and keratinocytes.

2. Mechanisms of the IL-31 Receptors

IL-31 plays a central role in innate and adaptive immune responses. The signaling triggered by most of these cytokines is mediated through their interaction with a novel cytokine receptor known as the gp130-like monocyte receptor or gp130-like receptor (GPL), which is a member of the type I cytokine receptor family [2]. IL-31 receptor (IL-31R) consists of two subunits, the IL-31 receptor alpha (IL-31RA) and OSM receptor

\beta{}

(OSMR

\beta{}

) [1, 2]. Receptor expression on the cells is upregulated by interferon-

\gamma{}

(IFN

\gamma{}

) and toll-like receptor 2/toll-like receptor 1 agonists [3]. IL-31 in turn stimulates the expression of the receptor itself, especially in synergy with IL-33 [4]. The binding of IL-31 to its receptor induces the activation of three principal signaling pathways: (i) the JAK/STAT pathway (Janus kinase/signal transducer and activator of transcription), (ii) the PI3K/AKT pathway (phosphatidylinositol 3’-kinase/protein kinase B), and (iii) the mitogen-activated protein kinase (MAPK) pathway, specifically involving c-Jun N-terminal kinase (JNK) and p38 mitogen-activated protein kinases. Furthermore, adaptor molecules such as Src homology and Collagen (Shc) and Src homology-2-containing protein tyrosine phosphatase 2 (SHP-2) are also recruited within this signaling cascade, contributing to the amplification of MAPK activation [1]. The interaction of IL-31 with its receptors and the consequent activation of signaling pathways including JAK/STAT, PI3K/AKT, and MAPK (JNK/p38) underscores its pro-inflammatory function, implicating IL-31 in the pathogenesis of multiple immune-mediated disorders as well as in tumor development.

3. Role of “IL-31/IL-33 Axis” in Immune-mediated Diseases and Cancer Pruritus

IL-31 controls the onset and maintenance of itching, mainly in atopic dermatitis (AD) and psoriasis (Pso) [4], favoring late onset of itching compared to histamine-induced itch [1, 4]. IL-31 through the phosphorylation of JAK1/2 and PI3K/AKT determines the activation of STAT3 and STAT5 inducing itching and Th-1-mediated skin keratinocyte cell proliferation, differentiation, apoptosis, and inflammation [1, 5]. Expression diversity is driven by microenvironment: autocrine expression of IL-4 activates Th1 cells to express IL-31 (Fig. 1). Various stimuli, including allergenic substances, infectious organisms, and UV radiation, can enhance the production of IL-31 [6].

Murdaca et al. [4] proposed the emerging idea of an IL-31/IL-33 interaction network possibly playing a role in the progression of allergic diseases, autoimmunity, and tumorigenesis. IL-33, a member of the “alarmins” family, is a nuclear cytokine produced by endothelial cells, epithelial cells, fibroblast-like cells, and myofibroblasts. It has been hypothesized that IL-33 may act both at an intracellular level as a nuclear factor regulating gene expression and at an extracellular level as a cytokine of the IL-1 family [7]. IL-33 is composed of two distinct domains: an N-terminal nuclear domain and a C-terminal IL-1-like cytokine domain, separated by a divergent central region. The IL-1 homologous region of IL-33 allows it to interact with soluble interleukin 1 receptor-like 1 (ST2), a membrane receptor classified within the Toll-like/IL-1 receptor group. This interaction facilitates association with the IL-1 receptor accessory protein (IL-1RAcP), which is shared among other IL-1 family members such as IL-1

\alpha{}

, IL-1

\beta{}

, and IL-36. ST2 is predominantly expressed on mast cells, group 2 innate lymphoid cells (ILC2), eosinophils, and regulatory T cells (Tregs), which constitute the primary cellular targets of IL-33 [5, 8].

Therefore, the involvement of the ‘IL-31/IL-33’ axis in allergic and autoimmune responses suggests a novel inflammatory mechanism, affirming IL-33’s role in initiating these responses [4, 9, 10, 11]. IL-31 activates a transcriptional program in sensory neurons that promotes neurite elongation and branching, thereby enhancing neuronal sensitivity to minimal stimuli and contributing to persistent pruritus [12].

Notably, itching is also a symptom of hematological tumorigenesis and cancers [13, 14]. IL-31 is expressed differently across multiple tumor categories and has the capacity to either promote or inhibit oncogenic advancement [15]. Akhtar et al. [16] discuss the current knowledge on the role of IL-31 in the pathogenesis of pruritus and in cancer onset and progression. They focus on the key role of Th2 cytokine (IL-4, IL-13, IL-25, IL-31, IL-33 and thymic stromal lymphopoietin) in mediating itch. In support of this theory, the authors point out that the administration of dupilumab (an antibody against IL-4

\alpha{}

, subunit of the receptor for IL-4 and IL-13) in patients with prostate cancer, cutaneous T-cell lymphoma and melanoma induced complete remission of itching altering the quality of life [17]. The positive effect of dupilumab is linked to the fact that the secretion of IL-31 is correlated with that of IL-4 and IL-13. The onset of itching must already be considered a negative indicator of the presence of cancer. First of all, itching could represent the first symptom, often unknown, of the development of a neoplasm and be determined by the action of factors released in the paraneoplastic syndrome. On the other hand, the presence of a tumor mass that takes up space could cause itching by stimulating nearby nerve fibers. Finally, antineoplastic drugs could stimulate the receptors leading to the onset of itching [13]. Imatinib mesylate, the first targeted therapy against chronic myeloid leukemia, induces the release of IL-33 which, by stimulating its receptor expressed on mast cells, determines the release of IL-31 resulting in the appearance of itching [18]. It should also be remembered that mantle cell lymphoma (MCL) is a pathology of advanced age where IL-33 levels are already higher than at a young age [18]. The elevated levels of IL-33 and the cutaneous infiltrate (“mass effect”) in mycosis fungoides and Sézary Syndrome explain the onset of pruritus which represents a hallmark symptom [18]. The importance of the “IL-31/IL-33 axis” in the onset of pruritus is confirmed by the positive therapeutic effect of dexamethasone, histone deacetylase inhibitors (midepsin and vorinostat) and mogamulizumab, a humanized monoclonal anti-CCR4 antibody. Mogamulizumab the suppresses IL-31+ Th2 cell subpopulation confirming that the “IL-31/IL-31RA axis” may be a possible therapeutic focus in patients with mycosis fungoides and Sézary Syndrome refractory to therapy for itching [16].

On the other hand, itching is also considered a negative signal of the progression of the neoplastic disease. Ferretti et al. [19] confirmed first of all that the intense pruritus in patients with Hodgkin Lymphoma is caused by IL-31 released by tumor-infiltrating Th2 cells which is capable of supporting a microenvironment stimulating the growth and diffusion of Hodgkin cells expressing IL-31R. Moreover, elevated levels of IL-31 maintain a microenvironment also favorable to the growth and spread of solid tumors. Indeed, in lung cancer high levels of IL-31 favor disease progression and dermal rash, pruritus, and xeroderma occurring in patients treated with epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (erlotinib and gefitinib) [20]. Akhtar et al. [16] confirmed in breast, gastric, colon, endometrial and ovarian cancers the role of IL-31 in cancer progression and the appearance of itching.

Single-nucleotide polymorphisms (SNPs) of the IL-31 gene may represent important information for cancer progression and survival. Indeed, the SNP rs7977932 of the IL-31 gene is correlated with endometrial-cancer susceptibility and the SNP rs4758680 with bladder cancer [1].

4. Conclusions

The use of monoclonal antibodies targeting IL-31 may not only serve as an effective tool for controlling itching and improving quality of life, but also as a strategy to limit tumor progression by supporting the action of antineoplastic drugs. Among the most recent innovations in the field of monoclonal anti-IL-31 therapies, Nemolizumab and Vixarelimab are the two that have passed phase II studies [21, 22].

Nemolizumab is a subcutaneously administered humanized monoclonal antibody targeting the IL-31RA, developed by Chugai Pharmaceutical Co., Ltd. It is approved for the treatment of pruritus associated with atopic dermatitis (ADaP), prurigo nodularis (PN), chronic kidney disease-associated pruritus (CKDaP), and systemic sclerosis (SSc) [23, 24].

Vixarelimab is also a human monoclonal antibody that is currently being studied for the treatment of PN alone. It acts at the level of the OSMR

\beta{}

receptor, simultaneously inhibiting the two cytokine pathways implicated in itching, inflammation, hyperkeratosis and fibrosis [25, 26].

It is plausible that further clinical studies including pharmacogenomics studies on SNPs will be able to confirm the role of the IL-31/IL-33 axis and pave the way for targeted therapies targeting IL-31 or IL-33.

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