2007
DOI: 10.1002/chem.200700141
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De Novo Synthesis of Uronic Acid Building Blocks for Assembly of Heparin Oligosaccharides

Abstract: An efficient de novo synthesis of uronic acid building blocks is described. The synthetic strategy relies on the stereoselective elongation of thioacetal protected dialdehydes 12 a and 17. The dialdehydes are prepared from D-xylose, a cheap and commercially available source. A highly stereoselective MgBr(2)OEt(2)-mediated Mukaiyama aldol addition to C4-aldehyde 12 a is performed to obtain D-glucuronic acid building block 16, whereas L-iduronic acid building block 22 is prepared by MgBr(2)OEt(2)-mediated cyanat… Show more

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Cited by 65 publications
(38 citation statements)
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“…ΔHexA(2S)-GlcN(NS,6S)-GlcAGlcN(NS,6S) ) Uronic acid building blocks for heparin oligosaccharides MALDI Synthesis by stereoselective elongation of thio-acetal protected dialdehydes (Adibekian, et al, 2007) N-linked glycans 13 C-Neu5Ac-labelled biantennary glycans MALDI Synthesised with [1,2,3,10,11-13 C]-CMP-β-Neu5Ac (Macnaughtan, et al, 2008) HexNAc-(Pent)HexA-(Pent)Hex-Hex-HexNAc-Asn…”
Section: Maldi (Dhb)mentioning
confidence: 99%
“…ΔHexA(2S)-GlcN(NS,6S)-GlcAGlcN(NS,6S) ) Uronic acid building blocks for heparin oligosaccharides MALDI Synthesis by stereoselective elongation of thio-acetal protected dialdehydes (Adibekian, et al, 2007) N-linked glycans 13 C-Neu5Ac-labelled biantennary glycans MALDI Synthesised with [1,2,3,10,11-13 C]-CMP-β-Neu5Ac (Macnaughtan, et al, 2008) HexNAc-(Pent)HexA-(Pent)Hex-Hex-HexNAc-Asn…”
Section: Maldi (Dhb)mentioning
confidence: 99%
“…Structural representation of (A and B) dialdehydes 1 and 2 (compounds 12a and 17 of reference ) utilized, respectively, for synthesis of (C) d ‐GlcA and (D) l ‐IdoA building blocks (compounds 16 and 22 of reference ). The abbreviation of protecting groups are as follows: Bn = benzil, Lev = levulinoyl, Me = methyl, Piv = pivaloyl, SEt = silyl ether.…”
Section: Synthetic Gagsmentioning
confidence: 99%
“…Particularly advantageous is the preparation of carbohydrate building blocks that can directly be used in the synthesis of oligosaccharides or other glycoconjugates without further protecting group transformations. [6] In this context, we recently described de novo approaches towards different classes of amino sugars and their mimetics starting from enantiopure 1,2-oxazines, [7] which are surprisingly versatile intermediates for the stereoselective synthesis of a variety of carbohydrate related compounds such as polyhydroxylated pyrrolidines, azetidines or polyols. [8] Among these differently configured C2-branched 4-amino sugars A have been generated from bicyclic compounds B by a sequence of glycosidation reaction, stereoselective carbonyl reduction and reductive cleavage of the N À O bond (Scheme 1).…”
Section: Introductionmentioning
confidence: 99%