Publication | Open Access
Antisense strategies for glycosylation engineering of Chinese hamster ovary (CHO) cells
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Citations
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References
1998
Year
EngineeringNovel GlycoproteinsGlycobiologyImmunologyCell CulturePolysaccharideImmunotherapyOligosaccharide BiosynthesisGlycosylation EngineeringGlycosylationCell-based Drug DeliveryAntisense StrategiesCell TraffickingBioconjugationCell EngineeringCell BiologyBiomolecular EngineeringDrug TargetingBiotechnologySlex SynthesisChinese HamsterMedicineCarbohydrate-protein Interaction
Novel glycoproteins, inaccessible by other techniques, can be obtained by metabolic engineering of the oligosaccharide biosynthesis pathway. Furthermore, alteration of cell-surface oligosaccharides can change the properties of receptors involved in cell-cell adhesion. Sialyl Lewis X (sLex) is a cell-surface oligosaccharide determinant which is specifically expressed on granulocytes and monocytes and which interacts with selectins to influence leukocyte trafficking, thrombosis, inflammation, and cancer. Antisense technology targeting fucosyltransferase VI (Fuc-TVI), an enzyme necessary for the synthesis of the sLex in engineered Chinese hamster ovary (CHO) cells, has reduced Fuc-TVI activity, sLex synthesis, and adhesion to endothelial cells. Antisense methodology to reduce targeted activity in oligosaccharide biosynthesis or other pathways is an important addition to CHO cell metabolic engineering capabilities.
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