| Literature DB >> 27911829 |
Matthew J Webber1,2, Eric A Appel1, Brittany Vinciguerra3, Abel B Cortinas4, Lavanya S Thapa1,2, Siddharth Jhunjhunwala1, Lyle Isaacs5, Robert Langer6,2,4,7,8, Daniel G Anderson6,2,4,7,8.
Abstract
The covalent modification of therapeutic biomolecules has been broadly explored, leading to a number of clinically approved modified protein drugs. These modifications are typically intended to address challenges arising in biopharmaceutical practice by promoting improved stability and shelf life of therapeutic proteins in formulation, or modifying pharmacokinetics in the body. Toward these objectives, covalent modification with poly(ethylene glycol) (PEG) has been a common direction. Here, a platform approach to biopharmaceutical modification is described that relies on noncovalent, supramolecular host-guest interactions to endow proteins with prosthetic functionality. Specifically, a series of cucurbit[7]uril (CB[7])-PEG conjugates are shown to substantially increase the stability of three distinct protein drugs in formulation. Leveraging the known and high-affinity interaction between CB[7] and an N-terminal aromatic residue on one specific protein drug, insulin, further results in altering of its pharmacological properties in vivo by extending activity in a manner dependent on molecular weight of the attached PEG chain. Supramolecular modification of therapeutic proteins affords a noncovalent route to modify its properties, improving protein stability and activity as a formulation excipient. Furthermore, this offers a modular approach to append functionality to biopharmaceuticals by noncovalent modification with other molecules or polymers, for applications in formulation or therapy.Entities:
Keywords: drug delivery; protein engineering; protein formulation; supramolecular chemistry
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Year: 2016 PMID: 27911829 PMCID: PMC5167179 DOI: 10.1073/pnas.1616639113
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205