Literature DB >> 17920720

Disulfide bridge based PEGylation of proteins.

Steve Brocchini1, Antony Godwin, Sibu Balan, Ji-won Choi, Mire Zloh, Sunil Shaunak.   

Abstract

PEGylation is a clinically proven strategy for increasing the therapeutic efficacy of protein-based medicines. Our approach to site-specific PEGylation exploits the thiol selective chemistry of the two cysteine sulfur atoms from an accessible disulfide. It involves two key steps: (1) disulfide reduction to release the two cystine thiols, and (2) bis-alkylation to give a three-carbon bridge to which PEG is covalently attached. During this process, irreversible denaturation of the protein does not occur. Mechanistically, the conjugation is conducted by a sequential, interactive bis-alkylation using alpha,beta-unsaturated-beta'-mono-sulfone functionalized PEG reagents. The combination of: - (a) maintaining the protein's tertiary structure after reduction of a disulfide, (b) bis-thiol selectivity of the PEG reagent, and (c) PEG associated steric shielding ensure that only one PEG molecule is conjugated at each disulfide. Our studies have shown that peptides, proteins, enzymes and antibody fragments can be site-specifically PEGylated using a native and accessible disulfide without destroying the molecules' tertiary structure or abolishing its biological activity. As the stoichiometric efficiency of our approach also enables recycling of any unreacted protein, it offers the potential to make PEGylated biopharmaceuticals as cost-effective medicines.

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Year:  2007        PMID: 17920720     DOI: 10.1016/j.addr.2007.06.014

Source DB:  PubMed          Journal:  Adv Drug Deliv Rev        ISSN: 0169-409X            Impact factor:   15.470


  26 in total

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5.  NMEGylation: a novel modification to enhance the bioavailability of therapeutic peptides.

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8.  Monovalent TNF receptor 1-selective antibody with improved affinity and neutralizing activity.

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9.  Utilizing Inverse Emulsion Polymerization To Generate Responsive Nanogels for Cytosolic Protein Delivery.

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10.  Protein modification, bioconjugation, and disulfide bridging using bromomaleimides.

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