| Literature DB >> 12612588 |
Steve Elliott1, Tony Lorenzini, Sheilah Asher, Ken Aoki, David Brankow, Lynette Buck, Leigh Busse, David Chang, Janis Fuller, James Grant, Natasha Hernday, Martha Hokum, Sylvia Hu, Andrew Knudten, Nancy Levin, Renee Komorowski, Frank Martin, Rachell Navarro, Timothy Osslund, Gary Rogers, Norma Rogers, Geri Trail, Joan Egrie.
Abstract
Delivery of protein therapeutics often requires frequent injections because of low activity or rapid clearance, thereby placing a burden on patients and caregivers. Using glycoengineering, we have increased and prolonged the activity of proteins, thus allowing reduced frequency of administration. Glycosylation analogs with new N-linked glycosylation consensus sequences introduced into the protein were screened for the presence of additional N-linked carbohydrates and retention of in vitro activity. Suitable consensus sequences were combined in one molecule, resulting in glycosylation analogs of rHuEPO, leptin, and Mpl ligand. All three molecules had substantially increased in vivo activity and prolonged duration of action. Because these proteins were of three different classes (rHuEPO is an N-linked glycoprotein, Mpl ligand an O-linked glycoprotein, and leptin contains no carbohydrate), glycoengineering may be generally applicable as a strategy for increasing the in vivo activity and duration of action of proteins. This strategy has been validated clinically for glycoengineered rHuEPO (darbopoetin alfa).Entities:
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Year: 2003 PMID: 12612588 DOI: 10.1038/nbt799
Source DB: PubMed Journal: Nat Biotechnol ISSN: 1087-0156 Impact factor: 54.908