Abstract

Pre-existing antibodies that bind polyethylene glycol are present in about 40% of healthy individuals. It is currently unknown if pre-existing anti-polyethylene glycol (PEG) antibodies can alter the bioactivity of pegylated drugs with a single long PEG chain, which represents the majority of newly developed pegylated medicines. Methoxy polyethylene glycol-epoetin beta (PEG-EPO) contains a single 30 kDa PEG chain and is used to treat patients suffering from anemia. We find that the pre-existing human anti-PEG IgM and IgG antibodies from normal donors can bind to PEG-EPO. The prevalence and concentrations of anti-PEG IgM and IgG antibodies were also higher in patients that responded poorly to PEG-EPO. Monoclonal anti-PEG IgM and IgG antibodies at concentrations found in normal donors blocked the biological activity of PEG-EPO to stimulate the production of new erythrocytes in mice and accelerated the clearance of 125I-PEG-EPO, resulting in PEG-EPO accumulation primarily in the liver and spleen. Accelerated clearance by the anti-PEG IgG antibody was mediated by the Fc portion of the antibody. Importantly, infusing higher doses of PEG-EPO could compensate for the inhibitory effects of anti-PEG antibodies, suggesting that pre-existing anti-PEG antibodies can be “dosed through.” Our study indicates that the bioactivity and therapeutic activity of PEG-EPO may be reduced in patients with elevated levels of pre-existing anti-PEG antibodies. New pegylated medicines with a single long PEG chain may also be affected in patients with high levels of anti-PEG antibodies.

Highlights

  • Polyethylene glycol (PEG) is often attached to proteins, peptides, nucleic acids, and nanoparticles to enhance water solubility, increase resistance to proteolytic enzymes, and reduce kidney excretion

  • To examine if serum samples containing pre-existing anti-polyethylene glycol (PEG) antibodies from healthy donors can bind to polyethylene glycol-epoetin beta (PEG-EPO), serial dilutions of donor plasma samples that tested positive for anti-PEG antibodies were added to ELISA plates coated with PEG-EPO

  • These results show that serum samples containing human anti-PEG IgM or IgG antibodies can bind PEG-EPO

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Summary

Introduction

Polyethylene glycol (PEG) is often attached to proteins, peptides, nucleic acids, and nanoparticles to enhance water solubility, increase resistance to proteolytic enzymes, and reduce kidney excretion. High levels of induced anti-PEG antibodies can alter the half-life and biological activity of pegylated drugs in patients [7,8,11,14]. PEG-EPO is modified with one linear 30 kDa PEG chain to extend its half-life (approximately 130 h), thereby allowing it to be administered intravenously or subcutaneously at prolonged dosing intervals. It is currently unknown if anti-PEG antibodies can alter the bioactivity of PEG-EPO. Our results suggest that pre-existing anti-PEG antibodies may alter the biological activity of PEG-EPO in some patients

Reagents
Ethical Statement
Plasma Sample Collection
Human Anti-PEG Antibody Assays
Clinical Relevance of Anemia Patients
Mouse Monoclonal Anti-PEG Antibody Assay
Immunoblotting
Measurement of Anti-PEG Antibodies in Mice Serum
Red Blood Cell Measurement
2.11. Biodistribution of 125I- PEG-EPO
2.12. Pharmacokinetics of 125I- PEG-EPO
2.14. Statistical Analysis
Pre-Existing Anti-PEG Antibodies in Healthy Donors Bind to PEG-EPO
Pre-Existing Anti-PEG Antibodies in Anemia Patients Receiving PEG-EPO
Anti-PEG Antibodies Can Decrease the Bioactivity of PEG-EPO in Mice
Anti-PEG Antibodies Promote PEG-EPO Accumulation in the Spleen and Liver
Anti-PEG Antibodies can Accelerate the Clearance of PEG-EPO in Mice
Fc-Mediated Clearance can be Compensated by Altering PEG-EPO Dose
Discussion
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