Scalable syntheses of both enantiomers of DNJNAc and DGJNAc from glucuronolactone: The effect of N-alkylation on hexosaminidase inhibition

Andreas F.G. Glawar; Daniel Best; Benjamin J. Ayers; Saori Miyauchi; Shinpei Nakagawa; Matilde Aguilar-Moncayo; José M. García Fernández; Carmen Ortiz Mellet; Elizabeth V. Crabtree; Terry D. Butters; Francis X. Wilson; Atsushi Kato; George W.J. Fleet

doi:10.1002/chem.201200110

Scalable syntheses of both enantiomers of DNJNAc and DGJNAc from glucuronolactone: The effect of N-alkylation on hexosaminidase inhibition

Andreas F.G. Glawar, Daniel Best, Benjamin J. Ayers, Saori Miyauchi, Shinpei Nakagawa, Matilde Aguilar-Moncayo, José M. García Fernández, Carmen Ortiz Mellet, Elizabeth V. Crabtree, Terry D. Butters, Francis X. Wilson, Atsushi Kato, George W.J. Fleet^*

^*Corresponding author for this work

Hospital Pharmacy

Research output: Contribution to journal › Article › peer-review

46 Scopus citations

Abstract

The efficient scalable syntheses of 2-acetamido-1,2-dideoxy-D-galacto- nojirimycin (DGJNAc) and 2-acetamido-1,2-dideoxy-D-gluco-nojirimycin (DNJNAc) from D-glucuronolactone, as well as of their enantiomers from L-glucuronolactone, are reported. The evaluation of both enantiomers of DNJNAc and DGJNAc, along with their N-alkyl derivatives, as glycosidase inhibitors showed that DGJNAc and its N-alkyl derivatives were all inhibitors of α-GalNAcase but that none of the epimeric DNJNAc derivatives inhibited this enzyme. In contrast, both DGJNAc and DNJNAc, as well as their alkyl derivatives, were potent inhibitors of β-GlcNAcases and β-GalNAcases. Neither of the L-enantiomers showed any significant inhibition of any of the enzymes tested. Correlation of the in vitro inhibition with the cellular data, by using a free oligosaccharide analysis of the lysosomal enzyme inhibition, revealed the following structure-property relationship: hydrophobic side-chains preferentially promoted the intracellular access of iminosugars to those inhibitors with more-hydrophilic side-chain characteristics. Getting the NAc of it: Scalable syntheses of DGJNAc and DNJNAc from D-glucuronolactone are reported. DGJNAc and its N-alkyl derivatives were inhibitors of α-GalNAcase and both DGJNAc and DNJNAc were potent inhibitors of β-GlcNAcases and β-GalNAcases.

Original language	English
Pages (from-to)	9341-9359
Number of pages	19
Journal	Chemistry - A European Journal
Volume	18
Issue number	30
DOIs	https://doi.org/10.1002/chem.201200110
State	Published - 2012/07/23

Keywords

carbohydrates
cell penetration
iminosugars
inhibitors
oligosaccharides

ASJC Scopus subject areas

General Chemistry
Catalysis
Organic Chemistry

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10.1002/chem.201200110

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Glawar, A. F. G., Best, D., Ayers, B. J., Miyauchi, S., Nakagawa, S., Aguilar-Moncayo, M., García Fernández, J. M., Ortiz Mellet, C., Crabtree, E. V., Butters, T. D., Wilson, F. X., Kato, A., & Fleet, G. W. J. (2012). Scalable syntheses of both enantiomers of DNJNAc and DGJNAc from glucuronolactone: The effect of N-alkylation on hexosaminidase inhibition. Chemistry - A European Journal, 18(30), 9341-9359. https://doi.org/10.1002/chem.201200110

@article{e98edceecdf04803821c29bac6949520,

title = "Scalable syntheses of both enantiomers of DNJNAc and DGJNAc from glucuronolactone: The effect of N-alkylation on hexosaminidase inhibition",

abstract = "The efficient scalable syntheses of 2-acetamido-1,2-dideoxy-D-galacto- nojirimycin (DGJNAc) and 2-acetamido-1,2-dideoxy-D-gluco-nojirimycin (DNJNAc) from D-glucuronolactone, as well as of their enantiomers from L-glucuronolactone, are reported. The evaluation of both enantiomers of DNJNAc and DGJNAc, along with their N-alkyl derivatives, as glycosidase inhibitors showed that DGJNAc and its N-alkyl derivatives were all inhibitors of α-GalNAcase but that none of the epimeric DNJNAc derivatives inhibited this enzyme. In contrast, both DGJNAc and DNJNAc, as well as their alkyl derivatives, were potent inhibitors of β-GlcNAcases and β-GalNAcases. Neither of the L-enantiomers showed any significant inhibition of any of the enzymes tested. Correlation of the in vitro inhibition with the cellular data, by using a free oligosaccharide analysis of the lysosomal enzyme inhibition, revealed the following structure-property relationship: hydrophobic side-chains preferentially promoted the intracellular access of iminosugars to those inhibitors with more-hydrophilic side-chain characteristics. Getting the NAc of it: Scalable syntheses of DGJNAc and DNJNAc from D-glucuronolactone are reported. DGJNAc and its N-alkyl derivatives were inhibitors of α-GalNAcase and both DGJNAc and DNJNAc were potent inhibitors of β-GlcNAcases and β-GalNAcases.",

keywords = "carbohydrates, cell penetration, iminosugars, inhibitors, oligosaccharides",

author = "Glawar, {Andreas F.G.} and Daniel Best and Ayers, {Benjamin J.} and Saori Miyauchi and Shinpei Nakagawa and Matilde Aguilar-Moncayo and {Garc{\'i}a Fern{\'a}ndez}, {Jos{\'e} M.} and {Ortiz Mellet}, Carmen and Crabtree, {Elizabeth V.} and Butters, {Terry D.} and Wilson, {Francis X.} and Atsushi Kato and Fleet, {George W.J.}",

year = "2012",

month = jul,

day = "23",

doi = "10.1002/chem.201200110",

language = "英語",

volume = "18",

pages = "9341--9359",

journal = "Chemistry - A European Journal",

issn = "0947-6539",

publisher = "Wiley-VCH Verlag",

number = "30",

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Glawar, AFG, Best, D, Ayers, BJ, Miyauchi, S, Nakagawa, S, Aguilar-Moncayo, M, García Fernández, JM, Ortiz Mellet, C, Crabtree, EV, Butters, TD, Wilson, FX, Kato, A & Fleet, GWJ 2012, 'Scalable syntheses of both enantiomers of DNJNAc and DGJNAc from glucuronolactone: The effect of N-alkylation on hexosaminidase inhibition', Chemistry - A European Journal, vol. 18, no. 30, pp. 9341-9359. https://doi.org/10.1002/chem.201200110

TY - JOUR

T1 - Scalable syntheses of both enantiomers of DNJNAc and DGJNAc from glucuronolactone

T2 - The effect of N-alkylation on hexosaminidase inhibition

AU - Glawar, Andreas F.G.

AU - Best, Daniel

AU - Ayers, Benjamin J.

AU - Miyauchi, Saori

AU - Nakagawa, Shinpei

AU - Aguilar-Moncayo, Matilde

AU - García Fernández, José M.

AU - Ortiz Mellet, Carmen

AU - Crabtree, Elizabeth V.

AU - Butters, Terry D.

AU - Wilson, Francis X.

AU - Kato, Atsushi

AU - Fleet, George W.J.

PY - 2012/7/23

Y1 - 2012/7/23

N2 - The efficient scalable syntheses of 2-acetamido-1,2-dideoxy-D-galacto- nojirimycin (DGJNAc) and 2-acetamido-1,2-dideoxy-D-gluco-nojirimycin (DNJNAc) from D-glucuronolactone, as well as of their enantiomers from L-glucuronolactone, are reported. The evaluation of both enantiomers of DNJNAc and DGJNAc, along with their N-alkyl derivatives, as glycosidase inhibitors showed that DGJNAc and its N-alkyl derivatives were all inhibitors of α-GalNAcase but that none of the epimeric DNJNAc derivatives inhibited this enzyme. In contrast, both DGJNAc and DNJNAc, as well as their alkyl derivatives, were potent inhibitors of β-GlcNAcases and β-GalNAcases. Neither of the L-enantiomers showed any significant inhibition of any of the enzymes tested. Correlation of the in vitro inhibition with the cellular data, by using a free oligosaccharide analysis of the lysosomal enzyme inhibition, revealed the following structure-property relationship: hydrophobic side-chains preferentially promoted the intracellular access of iminosugars to those inhibitors with more-hydrophilic side-chain characteristics. Getting the NAc of it: Scalable syntheses of DGJNAc and DNJNAc from D-glucuronolactone are reported. DGJNAc and its N-alkyl derivatives were inhibitors of α-GalNAcase and both DGJNAc and DNJNAc were potent inhibitors of β-GlcNAcases and β-GalNAcases.

AB - The efficient scalable syntheses of 2-acetamido-1,2-dideoxy-D-galacto- nojirimycin (DGJNAc) and 2-acetamido-1,2-dideoxy-D-gluco-nojirimycin (DNJNAc) from D-glucuronolactone, as well as of their enantiomers from L-glucuronolactone, are reported. The evaluation of both enantiomers of DNJNAc and DGJNAc, along with their N-alkyl derivatives, as glycosidase inhibitors showed that DGJNAc and its N-alkyl derivatives were all inhibitors of α-GalNAcase but that none of the epimeric DNJNAc derivatives inhibited this enzyme. In contrast, both DGJNAc and DNJNAc, as well as their alkyl derivatives, were potent inhibitors of β-GlcNAcases and β-GalNAcases. Neither of the L-enantiomers showed any significant inhibition of any of the enzymes tested. Correlation of the in vitro inhibition with the cellular data, by using a free oligosaccharide analysis of the lysosomal enzyme inhibition, revealed the following structure-property relationship: hydrophobic side-chains preferentially promoted the intracellular access of iminosugars to those inhibitors with more-hydrophilic side-chain characteristics. Getting the NAc of it: Scalable syntheses of DGJNAc and DNJNAc from D-glucuronolactone are reported. DGJNAc and its N-alkyl derivatives were inhibitors of α-GalNAcase and both DGJNAc and DNJNAc were potent inhibitors of β-GlcNAcases and β-GalNAcases.

KW - carbohydrates

KW - cell penetration

KW - iminosugars

KW - inhibitors

KW - oligosaccharides

UR - http://www.scopus.com/inward/record.url?scp=84863947375&partnerID=8YFLogxK

U2 - 10.1002/chem.201200110

DO - 10.1002/chem.201200110

M3 - 学術論文

C2 - 22736508

AN - SCOPUS:84863947375

SN - 0947-6539

VL - 18

SP - 9341

EP - 9359

JO - Chemistry - A European Journal

JF - Chemistry - A European Journal

IS - 30

ER -

Scalable syntheses of both enantiomers of DNJNAc and DGJNAc from glucuronolactone: The effect of N-alkylation on hexosaminidase inhibition

Abstract

Keywords

ASJC Scopus subject areas

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