1. High MW polyethylene glycol prolongs circulation of pegloticase in mice with anti-PEG antibodies
- Author
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Jonathan E. Frank, Zibo Li, Andrew C. Nyborg, Samuel K. Lai, Hong Yuan, Eric W. Livingston, Morgan D. McSweeney, Tao Zhang, Anne Talkington, and Brian LaMoreaux
- Subjects
Biodistribution ,Gout ,Urate Oxidase ,Pharmaceutical Science ,Polyethylene glycol ,Pharmacology ,Article ,Polyethylene Glycols ,Mice ,chemistry.chemical_compound ,PEG ratio ,medicine ,Animals ,Humans ,Tissue Distribution ,biology ,business.industry ,medicine.disease ,Uric Acid ,Titer ,Pegloticase ,chemistry ,Toxicity ,biology.protein ,Antibody ,business ,medicine.drug - Abstract
Pegloticase is an enzyme used to reduce serum uric acid levels in patients with chronic, treatment-refractory gout. Clinically, about 40% of patients develop high titers of anti-PEG antibodies (APA) after initial treatment, which in turn quickly eliminate subsequent doses of pegloticase from the systemic circulation and render the treatment ineffective. We previously found that pre-infusion with high MW free PEG (40 kDa) can serve as a decoy to saturate circulating APA, preventing binding to a subsequently administered dose of PEG-liposomes and restoring their prolonged circulation in mice, without any detectible toxicity. Here, we investigated the use of 40 kDa free PEG to restore the circulation of radio-labeled pegloticase in mice using longitudinal Positron Emission Tomography (PET) imaging over 4 days. Mice injected with pegloticase developed appreciable APA titers by Day 9, which further increased through Day 14. Compared to naive mice, mice with pegloticase-induced APA rapidly cleared 89Zr-labeled pegloticase, with ~75% lower pegloticase concentrations in the circulation at four hours after treatment. The 96-h AUC in APA+ mice was less than 30% of the AUC in naive mice. In contrast, pre-infusion of free PEG into PEG-sensitized mice restored the AUC of pegloticase to ~80% of that seen in naive mice, resulting in a similar biodistribution to pegloticase in naive mice over time. These results suggest that pre-infusion of free PEG may be a promising strategy to enable the safe and efficacious use of pegloticase and other PEGylated drugs in patients that have previously failed therapy due to induced APA.
- Published
- 2021
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