A Novel Human Interleukin‐23A Overexpressing Mouse Model of Systemic Lupus Erythematosus-Reference-Cited by-同舟云学术

A Novel Human Interleukin‐23A Overexpressing Mouse Model of Systemic Lupus Erythematosus

Published:2024-04-02 Issue:7 Volume:76 Page:1085-1095
ISSN:2326-5191
Container-title:Arthritis & Rheumatology
language:en
Short-container-title:Arthritis & Rheumatology

Author:

Christodoulou‐Vafeiadou Eleni¹,Geka Christina¹,Iliopoulou Lida²,Ntari Lydia¹,Denis Maria C.¹,Karagianni Niki¹,Kollias George³^ORCID

Affiliation:

1. Biomedcode Hellas SA Athens Greece

2. Biomedical Sciences Research Center (BSRC) Alexander Fleming Athens Greece

3. BSRC Alexander Fleming, Athens, Greece, and School of Medicine, National and Kapodistrian University of Athens Athens Greece

Abstract

ObjectiveInterleukin‐23 (IL‐23) is a crucial cytokine implicated in chronic inflammation and autoimmunity, associated with various diseases such as psoriasis, psoriatic arthritis, and systemic lupus erythematosus (SLE). This study aimed to create and characterize a transgenic mouse model overexpressing human IL‐23A (TghIL‐23A), providing a valuable tool for investigating the pathogenic role of human IL‐23A and evaluating the efficacy of anti–human IL‐23A therapeutics.MethodsTghIL‐23A mice were generated via microinjection of CBA × C57BL/6 zygotes with a fragment of the human IL23A gene, flanked by its 5′‐regulatory sequences and the 3′ untranslated region of human β‐globin. The TghIL‐23A pathology was assessed through hematologic and biochemic analyses, cytokine and antinuclear antibody detection, and histopathologic examination of skin and renal tissues. The response to the anti–human IL‐23A therapeutic agent guselkumab was evaluated in groups of eight mixed‐sex mice receiving subcutaneous treatment twice weekly for 10 weeks using clinical, biomarker, and histopathologic readouts.ResultsTghIL‐23A mice exhibited interactions between human IL‐23A and mouse IL‐23/IL‐12p40 and developed a chronic multiorgan autoimmune disease marked by proteinuria, anti–double‐stranded DNA antibodies, severe inflammatory lesions in the skin, and milder phenotypes in the kidneys and lungs. The TghIL‐23A pathologic features exhibited significant similarities to those observed in human patients with SLE, and they were reversed following guselkumab treatment.ConclusionWe have generated and characterized a novel genetic mouse model of SLE, providing proof‐of‐concept for the etiopathogenic role of human IL‐23A. This new model has a normal life span and integrates several characteristics of the human disease's complexity and chronicity, making it an attractive preclinical tool for studying IL‐23–dependent pathogenic mechanisms and assessing the efficacy of anti–human IL‐23A or modeled disease‐related therapeutics.

image

Publisher

Wiley

Reference46 articles.

1. Novel p19 Protein Engages IL-12p40 to Form a Cytokine, IL-23, with Biological Activities Similar as Well as Distinct from IL-12

2. Abundant expression of the interleukin (IL)23 subunit p19, but low levels of bioactive IL23 in the rheumatoid synovium: differential expression and Toll-like receptor-(TLR) dependent regulation of the IL23 subunits, p19 and p40, in rheumatoid arthritis

3. Synergism between tumor necrosis factor alpha and interleukin-17 to induce IL-23 p19 expression in fibroblast-like synoviocytes

4. Understanding the IL-23–IL-17 immune pathway

5. Role of the IL-23/IL-17 Pathway in Rheumatic Diseases: An Overview