Interleukin-13 neutralization by two distinct receptor blocking mechanisms reduces immunoglobulin E responses and lung inflammation in cynomolgus monkeys

被引:40
作者
Kasaian, Marion T. [2 ]
Tan, Xiang-Yang [1 ]
Jin, Macy [1 ]
Fitz, Lori [2 ]
Marquette, Kimberly [1 ]
Wood, Nancy [2 ]
Cook, Timothy A. [2 ]
Lee, Julie [2 ]
Widom, Angela [1 ]
Agostinelli, Rita [1 ]
Bree, Andrea [2 ]
Schlerman, Franklin J. [2 ]
Olland, Stephane [1 ]
Wadanoli, Michael [3 ]
Sypek, Joseph [2 ]
Gill, Davinder [1 ]
Goldman, Samuel J. [2 ]
Tchistiakova, Lioudmila [1 ]
机构
[1] Wyeth Res, Dept Biol Technol, Cambridge, MA 02140 USA
[2] Wyeth Res, Dept Inflammat, Cambridge, MA 02140 USA
[3] Wyeth Res, Dept Bioresources, Andover, MA USA
关键词
D O I
10.1124/jpet.108.136515
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Interleukin (IL)-13 is a key cytokine driving allergic and asthmatic responses and contributes to airway inflammation in cynomolgus monkeys after segmental challenge with Ascaris suum antigen. IL-13 bioactivity is mediated by a heterodimeric receptor (IL-13R alpha 1/IL-4R alpha) and can be inhibited in vitro by targeting IL-13 interaction with either chain. However, in cytokine systems, in vitro neutralization activity may not always predict inhibitory function in vivo. To address the efficacy of two different IL-13 neutralization mechanisms in a primate model of atopic disease, two humanized monoclonal antibodies to IL-13 were generated, with highly homologous properties, differing in epitope recognition. Ab01 blocks IL-13 interaction with IL-4R alpha, and Ab02 blocks IL-13 interaction with IL-13R alpha 1. In a cynomolgus monkey model of IgE responses to A. suum antigen, both Ab01 and Ab02 effectively reduced serum titers of Ascaris-specific IgE and diminished ex vivo Ascaris-triggered basophil histamine release, assayed 8 weeks after a single administration of antibody. The two antibodies also produced comparable reductions in pulmonary inflammation after lung segmental challenge with Ascaris antigen. Increased serum levels of IL-13, lacking demonstrable biological activity, were seen postchallenge in animals given either anti-IL-13 antibody but not in control animals given human IgG of irrelevant specificity. These findings demonstrate a potent effect of IL-13 neutralization on IgE-mediated atopic responses in a primate system and show that IL-13 can be efficiently neutralized by targeting either the IL-4R alpha-binding epitope or the IL-13R alpha 1-binding epitope.
引用
收藏
页码:882 / 892
页数:11
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