Abstract
Polyethylene glycol (PEG) is an inert, water soluble polymer, used for decades in pharmaceuticals. Although PEG is considered safe, concerns persist about the potential adverse effects of long-term exposure to PEG-containing therapies, specifically in children, following the introduction of PEGylated recombinant factor products used for the treatment of hemophilia. Given the absence of long-term surveillance data, and to evaluate the potential risk, we estimated PEG exposure in the pediatric population receiving PEGylated therapies with pediatric indications administered intravenously or intramuscularly. We used a range of pediatric weights and doses based on prescribing information (PI) or treatment guidelines. PIs and reporting websites were searched for information about adverse events (AEs). For a child weighing 50 kg on the highest prophylactic dose of a FVIII product, the range of total PEG exposure was 40–21,840 mg/year; for factor IX (FIX) products, the range was 13–1342 mg/year; and for other products, the range was 383–26,743 mg/year, primarily as a derivative excipient. No AE patterns attributable to PEG were found for any of these products, including potential renal, neurological, or hepatic AEs. Our analyses suggest the pediatric population has had substantial exposure to PEG for several decades, with no evidence of adverse consequences.
Highlights
Polyethylene glycol (PEG) is a chemically inert, amphiphilic polymer of ethylene diol units that can be manufactured in various sizes and molecular weights
Given the lack of long-term surveillance data of PEG exposures in children, we developed an alternative approach to help healthcare providers (HCPs) understand the magnitude of exposure to PEG and its potential toxicity for rurioctocog alfa pegol, and all other FDA-approved, pediatric-indicated parental therapies with conjugated, derivative, and/or excipient PEG
To evaluate potential PEG-related toxicity, we investigated all publicly available adverse events (AEs) for PEG-containing pediatric-indicated therapies with intravenous (IV) or intramuscular (IM) routes of administration to determine if there were any general trends or any AEs that might be related to vacuolation [13,14] in the central nervous system (CNS), kidney, or liver
Summary
Polyethylene glycol (PEG) is a chemically inert, amphiphilic polymer of ethylene diol units that can be manufactured in various sizes and molecular weights. There are 20 PEGylated therapies with diverse indications in clinical use in the United States and Europe [1,6,7,8]. PEGylation of biotherapeutics has been applied in many clinical disorders, including hemophilia A and B [1,7,10,11]. With respect to factor VIII (FVIII) replacement therapy in hemophilia A, Antihemophilic Factor (Recombinant), PEGylated (rurioctocog alfa pegol, BAX 855, SHP660; ADYNOVI®/ADYNOVATE®, Shire, Lexington, MA, USA) has a half-life that is 1.4–1.5 fold longer [6,11] than Antihemophilic Factor (Recombinant) (ADVATE®, Shire Lexington, MA, USA), allowing for two doses per week rather than three for prophylaxis [6,11,12]
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