Efficient Synthesis of the Lewis A Tandem Repeat

Kobayashi, Daisuke; Ueki, Akiharu; Yamaji, Tomoya; Nagao, Kazuya; Imamura, Akira; Ando, Hiromune; Kiso, Makoto; Ishida, Hideyuki

doi:10.3390/molecules21050614

Cited by 4 publications

(4 citation statements)

References 22 publications

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“…Glycosylations of acceptors 14 and 16 produced the best yields, even though 16 was not the least reactive. Likewise, when the same acceptor was glycosylated with different donors (e.g., acceptor 13 reacting with different donors 6−8; see entries 1, 2, and 9), the reactive donor (8) had the highest yield. Apparently, the presence of two OBn groups at O4 and O6 in GlcNTCA rendered 8 an excellent donor.…”

Section: ■ Results and Discussionmentioning

confidence: 99%

“…In contrast, chemical synthesis was shown to avoid the disadvantages and additionally to provide these biologically important oligosaccharides in a sufficient quantity with flexibility. Kobayashi et al , for example, recently synthesized the fucosylated oligosaccharide that contained four Le a -tandem repeats by using ( N -phenyl) trifluoroacetimidate donors with a convergent approach. These growing research efforts signify the urgency to produce type I-repeating oligomers.…”

Section: Introductionmentioning

confidence: 99%

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Threshold of Thioglycoside Reactivity Difference Is Critical for Efficient Synthesis of Type I Oligosaccharides by Chemoselective Glycosylation

Verma

et al. 2020

J. Org. Chem.

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Synthesis of type I LacNAc (Galβ1 → 3GlcNAc) oligosaccharides usually suffers from low yields. We herein report the efficient synthesis of type I LacNAc oligosaccharides by chemoselective glycosylation. With 16 relative reactivity values (RRVs) measured thiotoluenyl-linked disaccharide donors and acceptors, chemoselective glycosylations were investigated to obtain optimal conditions. In these reactions, the RRV difference between the donors and acceptors had to be more than 6311 to obtain type I LacNAc tetrasaccharides in 72–86% yields, with minimal occurrence of aglycon transfer. The threshold of RRV difference was further applied to plan the synthesis of longer glycans. Because it is challenging to measure the RRVs of tetrasaccharides, anomeric proton chemical shifts were utilized to predict the corresponding RRVs, which consequently explained the outcome of glycosylations for the synthesis of type I LacNAc hexasaccharides. The result supported the idea that elongation of glycan chains has to proceed from the reducing to the nonreducing end for a better yield.

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Section: ■ Results and Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Threshold of Thioglycoside Reactivity Difference Is Critical for Efficient Synthesis of Type I Oligosaccharides by Chemoselective Glycosylation

Verma

et al. 2020

J. Org. Chem.

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“…Nevertheless, false negative and false positive results are possible and precautions are needed in interpreting the data [7,10,11]. sLe a oligosaccharides and analogs have been synthesized chemically [15][16][17][18][19][20] or chemoenzymatically [21][22][23][24]. Chemoenzymatic synthesis of sLe a antigens by sialidase (e.g.…”

Section: Introductionmentioning

confidence: 99%

Facile chemoenzymatic synthesis of Lewis a (Lea) antigen in gram-scale and sialyl Lewis a (sLea) antigens containing diverse sialic acid forms

Tasnima

Yan

et al. 2019

Carbohydrate Research

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An efficient streamlined chemoenzymatic approach has been developed for gram-scale synthesis of Lewis a angtigen (Le a βProN 3 ) and a library of sialyl Lewis a antigens (sLe a βProN 3 ) containing different sialic acid forms. Intially, commercially available inexpensive N-acetylglucosamine (GlcNAc) was converted to its N′-glycosyl p-toluenesulfonohydrazide in one step. Followed by chemical glycosylation, GlcNAcβProN 3 was synthesized using this protecting group-free method in high yield (82%). Sequential one-pot multienzyme (OPME) β1-3-galactosylation of GlcNAcβProN 3 followed by OPME α1-4-fucosylation reactions produced target Le a βProN 3 in gram-scale. Structurally diverse sialic acid forms was successfully introduced using a OPME sialylation reaction containing a CMP-sialic acid synthetase and Pasteurella multocida α2-3sialyltransferase 1 (PmST1) mutant PmST1 M144D with or without a sialic acid aldolase to form sLe a βProN 3 containing naturally occurring or non-natural sialic acid forms in preparative scales.

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“…The first synthesis of Le a -tandem repeat was developed and reported by Ishida et al. in 2016 ( Scheme 7 ) ( 51 ). The fucose-containing trisaccharide 42 was derived from monosaccharide 41 through multiple protecting group manipulations, followed by two glycosylation steps.…”

Section: Synthesis Of Type-i Lacnac Repeating Oligosaccharidesmentioning

confidence: 99%

Synthesis of Type-I and Type-II LacNAc-Repeating Oligosaccharides as the Backbones of Tumor-Associated Lewis Antigens

Phang

Lin

2022

Front. Immunol.

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Type-I and Type-II LacNAc are Gal-GlcNAc disaccharides bearing a β1,3- or β1,4-linkage respectively. They exist as the backbones of Lewis antigens that are highly expressed in several cancers. Owing to the promise of developing carbohydrate-based anti-cancer vaccines, glycan synthesis at a large scale is indeed an important task. Synthesis of Type-I and Type-II tandem repeat oligomers has been hampered by the presence of GlcNAc residues. Particularly, N-protecting group plays a determining role in affecting glycosyl donor’s reactivity and acceptor’s nucleophilicity. This review discusses several representative studies that assembled desirable glycans in an efficient manner, such as chemoselective one-pot synthesis and chemoenzymatic methods. Additionally, we also highlight solutions that have been offered to tackle long-lasting problems, e.g., prevention of the oxazoline formation and change of donor/acceptor reactivity. In retrospect of scientific achievements, we present the current restrictions and remaining challenges in this less explored frontier.

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Efficient Synthesis of the Lewis A Tandem Repeat

Cited by 4 publications

References 22 publications

Threshold of Thioglycoside Reactivity Difference Is Critical for Efficient Synthesis of Type I Oligosaccharides by Chemoselective Glycosylation

Threshold of Thioglycoside Reactivity Difference Is Critical for Efficient Synthesis of Type I Oligosaccharides by Chemoselective Glycosylation

Facile chemoenzymatic synthesis of Lewis a (Lea) antigen in gram-scale and sialyl Lewis a (sLea) antigens containing diverse sialic acid forms

Synthesis of Type-I and Type-II LacNAc-Repeating Oligosaccharides as the Backbones of Tumor-Associated Lewis Antigens

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