Original Articles: Basic and Clinical Immunology
Preclinical efficacy and safety of mepolizumab (SB-240563), a humanized monoclonal antibody to IL-5, in cynomolgus monkeys,☆☆

https://doi.org/10.1067/mai.2001.116576Get rights and content

Abstract

Background: Allergic respiratory diseases are characterized by large numbers of eosinophils and their reactive products in airways and blood; these are believed to be involved in progressive airway damage and remodeling. IL-5 is the principal cytokine for eosinophil maturation, differentiation, and survival. Mepolizumab (SB-240563), a humanized monoclonal antibody (mAb) specific for human IL-5, is currently in clinical trials for treatment of asthma. Objective: The purpose of this study was to characterize the pharmacologic activity and long-term safety profile of an anti–human IL-5 mAb to support clinical trials in asthmatic patients. Methods: Naive and Ascaris suum –sensitive cynomolgus monkeys received various dose levels of mepolizumab and were monitored for acute and chronic pharmacologic and toxic responses. Results: To support preclinical safety assessment, cynomolgus monkey IL-5 was cloned, expressed, and characterized. Although monkey IL-5 differs from human IL-5 by 2 amino acids (Ala27Gly and Asn40His), mepolizumab has comparable inhibitory activity against both monkey IL-5 and human IL-5. In A suum –sensitive monkeys, single doses of mepolizumab significantly reduced blood eosinophilia, eosinophil migration into lung airways, and levels of RANTES and IL-6 in lungs for 6 weeks. However, mepolizumab did not affect acute bronchoconstrictive responses to inhaled A suum . In an IL-2–induced eosinophilia model (up to 50% blood eosinophilia), 0.5 mg/kg mepolizumab blocked eosinophilia by >80%. Single-dose and chronic (6 monthly doses) intravenous and subcutaneous toxicity studies in naive monkeys found no target organ toxicity or immunotoxicity up to 300 mg/kg. Monkeys did not generate anti-human IgG antibodies. Monthly mepolizumab doses greater than 5 mg/kg caused an 80% to 100% decrease in blood and bronchoalveolar lavage eosinophils lasting 2 months after dosing, and there was no effect on eosinophil precursors in bone marrow after 6 months of treatment. Eosinophil decreases correlated with mepolizumab plasma concentrations (half-life = 13 days). Conclusion: These studies demonstrate that chronic antagonism of IL-5 by mepolizumab in monkeys is safe and has the potential, through long-term reductions in circulating and tissue-resident eosinophils, to be beneficial therapy for chronic inflammatory respiratory diseases. (J Allergy Clin Immunol 2001;108:250-7.)

Section snippets

Materials and methods

Mepolizumab was constructed through use of conventional molecular techniques to graft complementarity-determining regions from a parent murine mAb 2B6,16 raised against recombinant human (rh) IL-5, into human IgG1 (κ) heavy and light chains. Additional amino acid substitutions were made to reflect human immunoglobulin group/subgroup preferences. Mepolizumab’s binding affinity (Kd) for rhIL-5 is 4.2 pM. A stable Chinese hamster ovary cell line producing multigram quantities and a purification

Results

Initial evaluation of mepolizumab activity against IL-5 from various animal species used for pharmacology and toxicology studies (mouse, rat, guinea pig, dog, and monkey) found that mepolizumab would recognize and neutralize only IL-5 from primates. To compare mepolizumab’s activity against human IL-5 and its activity against monkey IL-5, cynomolgus monkey (Macaca fascicularis ) IL-5 was cloned and expressed. The amino acid sequence of monkey IL-5 differs from human IL-5 by 2 conservative

Discussion

In studies of mepolizumab in monkeys, in vivo pharmacologic activity leading to decreases in eosinophil counts was observed. In a 2-dose study, doses at or greater than 5 mg/kg produced a decrease of up to 85% in basal peripheral blood eosinophil counts as early as 8 days after the first dose. Counts remained >85% below control values for at least 11 weeks in monkeys that received 5 mg/kg or greater. Interestingly, after a second administration, doses at or greater than 0.5 mg/kg blocked

Acknowledgements

We gratefully acknowledge the assistance and support of Rodd Polsky, Charles Hottenstein, Kim Dede, Jeremy Harrop, Carol Silverman, Donna Cusimano, Elizabeth Gore, Donna Williams, Melanie Quinlan, Richard Macia, Gary Gries, and Mike Semanik in the conduct of this work. We also thank Drs John White and Charles Davis for their helpful discussions over the course of the studies reported here.

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    Funded by GlaxoSmithKline Pharmaceuticals.

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