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The creation of a tunable half-life technology
October 9, 2012
By: Mark Perkins
Novozymes Biopharma
Pharmaceutical companies are under ever increasing pressure to develop more novel, tailored drugs, while taking new therapeutics through clinical trials to market faster. As a result, the industry is seeing heavy investment in the development of biological drugs, which take much more targeted approaches to the treatment of diseases. A common challenge when using biological drugs is that they are often hampered by short plasma half-lives which can lead to reduced bioavailability, meaning that the human body clears the drug in a matter of minutes or hours. Consequently, patients with chronic conditions require higher dosages and more frequent administration of medications, resulting in the increased likelihood of side effects, greater healthcare costs and, inevitably, reduced patient compliance. Over recent years there has been much progress in the industry around developing technologies that can address the challenges and enable the serum half-life of protein-based therapeutics to be extended. Current strategies used are those that increase hydrodynamic volume (PEGylation) or those that use FcRn-mediated recycling (albumin fusions). Although current techniques have been successful in extending serum half-life, the ability to design protein half-life to deliver the required pharmacokinetics has not been possible. In response to the issue, a new half-life extension technology has recently been developed to offer a flexible drug delivery platform based on albumin, a natural non-immunogenic plasma protein with a proven and safe regulatory profile that allows manufacturers to tune protein or peptide half-life to specific medical needs. Through subtle modification of the albumin molecule, the new technology enables researchers to flexibly optimize and manage the pharmacokinetics of a target protein while retaining efficiency. Innovations in Technology Serum albumin displays a long half-life of 19 days in humans, in contrast to protein therapeutics, which are usually cleared from the body within a matter of minutes or hours. Apart from its size, it is the pH-dependent recycling through the neonatal FcRn receptor that protects albumin from renal clearance and is responsible for its extended half-life. Like IgGs, albumin is taken up by cells through nonspecific pinocytosis and is protected from intracellular degradation through pH-dependant binding to the FcRn in acidic endosomes. This interaction with the FcRn allows albumin to then be recycled back to the cell surface where it is released into circulation due to the physiological pH of the blood (Figure 1). Figure 1: Hypothetical model based on knowledge of IgG recycling. The neonatal Fc receptor (FcRn) functions to protect albumin from degradation resulting in prolonged half-life.
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