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

  • MAbs. 2017 Oct;9(7):1143-1154. doi: 10.1080/19420862.2017.1353853.
Rajkumar Ganesan  1 Ernest L Raymond  1 Detlev Mennerich  1 Joseph R Woska Jr  1 Gary Caviness  1 Christine Grimaldi  1 Jennifer Ahlberg  1 Rocio Perez  1 Simon Roberts  1 Danlin Yang  1 Kavita Jerath  1 Kristopher Truncali  1 Lee Frego  1 Eliud Sepulveda  1 Priyanka Gupta  1 Su-Ellen Brown  1 Michael D Howell  1 Keith A Canada  1 Rachel Kroe-Barrett  1 Jay S Fine  1 Sanjaya Singh  1 M Lamine Mbow  1
Affiliations
  • 1. a Boehringer Ingelheim Pharmaceuticals Inc. , Ridgefield , CT ., USA.
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.

Keywords
Generalized Pustular Psoriasis; IL-36R; IL1R family; IL1RL2; antagonist antibody.
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