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Down-regulated expression of plant-specific glycoepitopes in alfalfa
Authors:Sourrouille Christophe  Marquet-Blouin Estelle  D'Aoust Marc-André  Kiefer-Meyer Marie-Christine  Seveno Martial  Pagny-Salehabadi Sophie  Bardor Muriel  Durambur Gaelle  Lerouge Patrice  Vezina Louis  Gomord Véronique
Institution:CNRS UMR 6037, IFRMP 23, GDR 2590, Universitéde Rouen, 76821 Mont Saint Aignan, France;
Medicago Inc, 1020 Route de l'église, Bureau 600, Quebec, QC, Canada, G1V 3V9
Abstract:Compared with other plant expression systems used for pharmaceutical protein production, alfalfa offers the advantage of very homogeneous N -glycosylation. Therefore, this plant was selected for further attempts at glycoengineering. Two main approaches were developed in order to humanize N -glycosylation in alfalfa. The first was a knock-down of two plant-specific N -glycan maturation enzymes, β1,2-xylosyltransferase and α1,3-fucosyltransferases, using sense, antisense and RNA interference strategies. In a second approach, with the ultimate goal of rebuilding the whole human sialylation pathway, human β1,4-galactosyltransferase was expressed in alfalfa in a native form or in fusion with a targeting domain from N -acetylglucosaminyltransferase I, a glycosyltransferase located in the early Golgi apparatus in Nicotiana tabacum . Both knock-down and knock-in strategies strongly, but not completely, inhibited the biosynthesis of α1,3-fucose- and β1,2-xylose-containing glycoepitopes in transgenic alfalfa. However, recombinant human β1,4-galactosyltransferase activity in transgenic alfalfa completely prevented the accumulation of the Lewis a glycoepitope on complex N -glycans.
Keywords:alfalfa  glycoengineering  glycosyltransferase  Lewis a epitope                N-glycosylation  plant-made pharmaceutical
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