PO.PR02.01 · 预防研究
Development of a humanized IL-17A/IL-17F mouse model for preclinical efficacy studies of IL-17-related diseases
作者与单位
摘要 Abstract
Background: IL-17 cytokine family members exert diverse biological functions, promoting protective immunity against many pathogens while also driving inflammatory pathology in infection and autoimmunity. The IL-17 pathway has therefore become a major therapeutic target in autoimmune and chronic inflammatory disorders such as rheumatoid arthritis, multiple sclerosis, and psoriasis. Therapeutic monoclonal antibodies targeting IL-17A, IL-17A/IL-17F, the IL-17 receptor, or IL-23 have demonstrated substantial clinical efficacy in several of these conditions. In this study, we developed a novel humanized IL-17A/IL-17F mouse model and established an imiquimod (IMQ) -induced psoriasis model to evaluate the preclinical efficacy of bimekizumab and other test articles.
Methods: The hIL-17A/hIL-17F dual knockin mice were generated by homologous recombination, replacing the entire coding sequences of mouse I l -17 a and I l -17 f with their human counterparts while preserving the endogenous murine signal peptides. Human IL-17A and IL-17F mRNA transcription was validated by qRT-PCR, and corresponding serum protein levels were quantified by ELISA. Finally, topical IMQ application was used to trigger psoriasiform dermatitis on the back and ear skin of the hIL-17A/hIL-17F dual knockin mice. Bimekizumab and additional test agents were administered, and in vivo efficacy was assessed by H&E staining, pathological scoring, and cytokine profiling.
Results and Conclusion: IMQ treatment induced a psoriasis-like phenotype in hIL-17A/hIL-17F mice and resulted in high expression of human IL-17F. Bimekizumab and the test articles markedly improved histopathological features and reduced the levels of IL-17F in our mice. Overall, these findings demonstrate that the hIL-17A/hIL-17F dual humanized mouse provides an advanced tool for preclinical efficacy studies of IL-17-related therapeutics.
利益披露 Disclosure
H. He,
Shanghai Model Organisms Center, Inc. Other, Parent company.
A. Yang,
Shanghai Model Organisms Center, Inc. Other, Parent company.
S. Li,
Shanghai Model Organisms Center, Inc. Other, Parent company.
Q. Qi,
Shanghai Model Organisms Center, Inc. Other, Parent company.
Y. Li,
Shanghai Model Organisms Center, Inc. Other, Parent company.
R. Sun,
Shanghai Model Organisms Center, Inc. Other, Parent company.