Membrane-enclosed multienzyme (MEME) synthesis of 2,7-anhydro-sialic acid derivatives
Naturally occurring 2,7-anhydro-alpha-N-acetylneuraminic acid (2,7-anhydro-Neu5Ac) is a transglycosylation product of bacterial intramolecular trans-sialidases (IT-sialidases). A facile one-pot two-enzyme approach has been established for the synthesis of 2,7-anhydro-sialic acid derivatives includin...
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Veröffentlicht in: | Carbohydrate research 2017-11, Vol.451, p.110-117 |
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Sprache: | eng |
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Zusammenfassung: | Naturally occurring 2,7-anhydro-alpha-N-acetylneuraminic acid (2,7-anhydro-Neu5Ac) is a transglycosylation product of bacterial intramolecular trans-sialidases (IT-sialidases). A facile one-pot two-enzyme approach has been established for the synthesis of 2,7-anhydro-sialic acid derivatives including those containing different sialic acid forms such as Neu5Ac and N-glycolylneuraminic acid (Neu5Gc). The approach is based on the use of Ruminoccocus gnavus IT-sialidase for the release of 2,7-anhydro-sialic acid from glycoproteins, and the conversion of free sialic acid by a sialic acid aldolase. This synthetic method, which is based on a membrane-enclosed enzymatic synthesis, can be performed on a preparative scale. Using fetuin as a substrate, high-yield and cost-effective production of 2,7-anhydro-Neu5Ac was obtained to high-purity. This method was also applied to the synthesis of 2,7-anhydro-Neu5Gc. The membrane-enclosed multienzyme (MEME) strategy reported here provides an efficient approach to produce a variety of sialic acid derivatives.
Membrane-enclosed multienzyme (MEME) approach for the production of 2,7-anhydro-sialic acid derivatives. [Display omitted]
•A novel membrane enclosed multiple enzyme approach was developed for the production of 2,7-anhydro-sialic acid derivatives.•2,7-anhydro-Neu5Ac was produced in high-yield and high-purity.•Neu5Gc-rich glycoprotein was produced using a one-pot two-step enzymatic synthesis.•The method allowed the synthesis of a novel compound, 2,7-anhydro-Neu5Gc. |
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ISSN: | 0008-6215 1873-426X |
DOI: | 10.1016/j.carres.2017.08.008 |