Abstract
Despite the potential for the chemokine class as therapeutic targets in immune mediated disease, success has been limited. Many chemokines can bind to multiple receptors and many receptors have multiple ligands, with few exceptions. One of those exceptions is CCL20, which exclusively pairs to CCR6 and is associated with several immunologic conditions, thus providing a promising therapeutic target. Following successful evaluation in a single dose, first time in human clinical study, GSK3050002-a humanized IgG1 monoclonal antibody against human CCL20-was evaluated in a 26-week cynomolgus monkey toxicology study. A high incidence of unexpected vascular and organ inflammation was observed microscopically, leading to the decision to halt clinical development. Here we report a dose-responsive increase in the incidence and severity of inflammation in multiple organs from monkeys receiving 30 and 300 mg/kg/week by either subcutaneous or intravenous injection. Histomorphological changes resembled an immune complex-mediated pathology, which is often due to formation of anti-drug antibodies in monkeys receiving a human protein therapeutic and thus not predictive of clinical outcome. However, the presentation was atypical in that there was a clear dose response with a very high incidence of inflammation with a low incidence of ADA that did not correlate well individually. Additionally, the immunohistologic presentation was atypical in that the severity and distribution of tissue inflammation was greater than the numbers of associated immune complexes (i.e., granular deposits). An extensive ex vivo analysis of large molecular weight protein complexes in monkey serum from this study and in human serum samples demonstrated a time-dependent aggregation of GSK3050002, that was not predicted by in vitro assays. The aggregates also contained complement components. These findings support the hypothesis that immune complexes of drug aggregates, not necessarily including anti-drug antibodies, can fix complement, accumulate over time, and trigger immune complex disease. A situation which may have increased clinical relevance than typical anti-drug antibody-associated immune complex disease in monkeys administered human antibody proteins.
Highlights
Chemokines and chemokine receptors drive leukocyte recruitment and play an important role in inflammation and inflammatory diseases
The toxicology of GSK3050002 was evaluated in cynomolgus monkeys by weekly IV or SC administration of GSK3050002 at 30 mg/kg or 300 mg/kg weekly dosing for 26 weeks followed by a 12 week off-dose period
Drug aggregate induced immune complex disease complexes within tissues can result in generalised and/or localised pathology, including liver and kidney when immune complexes are cleared from circulation
Summary
Chemokines and chemokine receptors drive leukocyte recruitment and play an important role in inflammation and inflammatory diseases. GSK3050002 was evaluated in a first time in human single dose escalation clinical trial in which 36 healthy male subjects were exposed to single doses up to 20 mg/kg intravenously (IV). This study assessed safety, tolerability, pharmacokinetics and pharmacodynamics of GSK3050002 in healthy male volunteers. To support a longer duration clinical trial in patients, GSK3050002 was evaluated in a 26-week toxicology study in cynomolgus macaques. The cynomolgus monkey was chosen as a pharmacologically relevant animal species for nonclinical safety evaluation of GSK3050002. Two toxicology studies were completed with GSK3050002 in cynomolgus monkeys prior to the 26-week study described. Additional investigations were performed to understand the underlying mechanism of the observed pathology and comparisons were drawn between findings in monkeys and analysis of ex vivo samples from the first time in human clinical study with GSK3050002
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