Your search keyword '"antagonist antibody"' showing total 3 results

1. Generation and characterization of QLS22001, a humanized monoclonal antibody that neutralizes IL-17A and IL-17F with an extended half-life.

Author

Ma, Huimin, Zhang, Wei, Liu, Ke, Xu, Baoxin, Li, Minyu, Meng, Qingyun, An, Zhenming, and Chen, Bo

Subjects

*MONOCLONAL antibodies, *KRA, *T helper cells, *PSORIATIC arthritis, *KERATINOCYTES, *SPONDYLOARTHROPATHIES

Abstract

• QLS22001: a highly selective humanized monoclonal antibody with extended half-life. • QLS22001 neutralizes both IL-17A and IL-17F. • QLS22001 effectively blocks IL-17A and IL-17F mediated signaling pathway. • By introducing "YTE" to the Fc region of QLS22001, the half-life increases. • QLS22001a potential best-in-class therapeutic molecule for treatment of psoriasis. Therapeutic intervention to block IL-17A signaling has proven to be an effective treatment for numerous autoimmune diseases, including psoriasis, psoriatic arthritis, and axial spondylarthritis. Among the IL-17 family members, IL-17F, which shares 55% sequence homology with IL-17A, has been reported to functionally overlap with IL-17A in many inflammatory diseases. In this study, we describe the generation and characterization of QLS22001, a humanized monoclonal IgG1 antibody with an extended half-life and high affinity for both IL-17A and IL-17F. QLS22001 effectively blocks IL-17A and IL-17F mediated signaling pathways both in vitro and in vivo. Briefly, the YTE (M225Y/S254T/T256E) modification was introduced into the Fc fragment of QLS22001 WT Fc to prolong its half-life, and the resulting construct was named QLS22001. Functionally, it significantly inhibits IL-17A- and IL-17F-stimulated signaling in cell-based IL-6 release and reporter assays. The dual neutralization of the endogenous IL-17A and IL-17F produced by Th17 cells, as opposed to the selective blockade of IL-17A alone, results in a greater suppression of inflammatory cytokine secretion, according to in vitro blockade assays. Furthermore, in an in vivo mouse pharmacodynamic study, QLS22001 blocked human IL-17A-induced mouse keratinocyte chemoattractant (KC) release. In cynomolgus monkey pharmacokinetics evaluation, QLS22001 showed linear pharmacokinetic characteristics with a mean half-life of 31.2 days, while its parent antibody, QLS22001 WT Fc, had a mean half-life of 17.2 days. In addition, QLS22001 does not induce cytokine release in a human whole-blood assay. Collectively, these data provide a comprehensive preclinical characterization of QLS22001 and support its clinical development. [ABSTRACT FROM AUTHOR]

Published

2023

2. Generation and functional characterization of anti-human and anti-mouse IL-36R antagonist monoclonal antibodies

Author

Detlev Mennerich, Priyanka Gupta, Joseph R. Woska, Keith Canada, Danlin Yang, Michael D. Howell, Ernest L. Raymond, Rachel Kroe-Barrett, Gary O. Caviness, Rajkumar Ganesan, Simon Roberts, Kristopher Truncali, Su-Ellen Brown, Jennifer Ahlberg, M. Lamine Mbow, Jay S. Fine, Eliud Sepulveda, Sanjaya Singh, Perez Rocio K, Lee Frego, Kavita Jerath, and Christine Grimaldi

Subjects

0301 basic medicine, IL-36R, medicine.drug_class, medicine.medical_treatment, Immunology, Inflammation, Biology, Monoclonal antibody, Mice, 03 medical and health sciences, Antibody Specificity, Cell surface receptor, Report, Psoriasis, medicine, Animals, Humans, Immunology and Allergy, Receptor, IL1R family, Antibodies, Monoclonal, Receptors, Interleukin, medicine.disease, Receptor antagonist, antagonist antibody, 030104 developmental biology, Cytokine, Cancer research, Generalized pustular psoriasis, Generalized Pustular Psoriasis, medicine.symptom, IL1RL2

Abstract

Deficiency of interleukin (IL)-36 receptor antagonist (DITRA) syndrome is a rare autosomal recessive disease caused by mutations in IL36RN. IL-36R is a cell surface receptor and a member of the IL1R family that is involved in inflammatory responses triggered in skin and other epithelial tissues. Accumulating evidence suggests that IL-36R signaling may play a role in the pathogenesis of psoriasis. Therapeutic intervention of IL-36R signaling offers an innovative treatment paradigm for targeting epithelial cell-mediated inflammatory diseases such as the life-threatening psoriasis variant called generalized pustular psoriasis (GPP). We report the discovery and characterization of MAB92, a potent, high affinity anti-human IL-36 receptor antagonistic antibody that blocks human IL-36 ligand (α, β and γ)-mediated signaling. In vitro treatment with MAB92 directly inhibits human IL-36R-mediated signaling and inflammatory cytokine production in primary human keratinocytes and dermal fibroblasts. MAB92 shows exquisite species specificity toward human IL-36R and does not cross react to murine IL-36R. To enable in vivo pharmacology studies, we developed a mouse cross-reactive antibody, MAB04, which exhibits overlapping binding and pharmacological activity as MAB92. Epitope mapping indicates that MAB92 and MAB04 bind primarily to domain-2 of the human and mouse IL-36R proteins, respectively. Treatment with MAB04 abrogates imiquimod and IL-36-mediated skin inflammation in the mouse, further supporting an important role for IL-36R signaling in epithelial cell-mediated inflammation.

Published

2017

3. Generation and functional characterization of anti-human and anti-mouse IL-36R antagonist monoclonal antibodies.

Author

Ganesan R, Raymond EL, Mennerich D, Woska JR Jr, Caviness G, Grimaldi C, Ahlberg J, Perez R, Roberts S, Yang D, Jerath K, Truncali K, Frego L, Sepulveda E, Gupta P, Brown SE, Howell MD, Canada KA, Kroe-Barrett R, Fine JS, Singh S, and Mbow ML

Subjects

Animals, Antibody Specificity, Humans, Mice, Psoriasis immunology, Antibodies, Monoclonal immunology, Receptors, Interleukin antagonists & inhibitors

Abstract

Deficiency of interleukin (IL)-36 receptor antagonist (DITRA) syndrome is a rare autosomal recessive disease caused by mutations in IL36RN. IL-36R is a cell surface receptor and a member of the IL1R family that is involved in inflammatory responses triggered in skin and other epithelial tissues. Accumulating evidence suggests that IL-36R signaling may play a role in the pathogenesis of psoriasis. Therapeutic intervention of IL-36R signaling offers an innovative treatment paradigm for targeting epithelial cell-mediated inflammatory diseases such as the life-threatening psoriasis variant called generalized pustular psoriasis (GPP). We report the discovery and characterization of MAB92, a potent, high affinity anti-human IL-36 receptor antagonistic antibody that blocks human IL-36 ligand (α, β and γ)-mediated signaling. In vitro treatment with MAB92 directly inhibits human IL-36R-mediated signaling and inflammatory cytokine production in primary human keratinocytes and dermal fibroblasts. MAB92 shows exquisite species specificity toward human IL-36R and does not cross react to murine IL-36R. To enable in vivo pharmacology studies, we developed a mouse cross-reactive antibody, MAB04, which exhibits overlapping binding and pharmacological activity as MAB92. Epitope mapping indicates that MAB92 and MAB04 bind primarily to domain-2 of the human and mouse IL-36R proteins, respectively. Treatment with MAB04 abrogates imiquimod and IL-36-mediated skin inflammation in the mouse, further supporting an important role for IL-36R signaling in epithelial cell-mediated inflammation.

Published

2017