C2-Oxyanion Neighboring Group Participation: Transition State Structure for the Hydroxide-Promoted Hydrolysis of 4-Nitrophenyl α-<scp>d</scp>-Mannopyranoside

Speciale, Gaetano; Farren-Dai, Marco; Shidmoossavee, Fahimeh S.; Williams, Spencer J.; Bennet, Andrew J.

doi:10.1021/jacs.6b07935

Cited by 32 publications

(46 citation statements)

References 62 publications

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“…This process has little biological precedent (for a related proposal see Ref. ), but occurs in the base‐promoted solvolysis of α‐mannosides …”

Section: Introductionmentioning

confidence: 99%

“…[11]), but occurs in the base-promoted solvolysis of a-mannosides. [12] Efforts to develop inhibitors of GH99 enzymes have relied upon appending 1,3-linked a-glucosyl (to target mammalian endo-a-1,2-mannosidases) or 1,3-linked a-mannosyl (to target bacterial endo-a-1,2-mannanases) groups to various sugarshapedh eterocycles. Spiro and co-workersr eportedt he discoveryo fa-glucosyl-1,3-deoxymannojirimycin (GlcDMJ) as an effective inhibitor of the mammalian enzyme, [13,14] and followon studies by Fleet and co-workersr evealed a-mannosyl-1,3deoxymannojirimycin (ManDMJ) to be as lightly weaker inhibitor for this enzyme ( Figure 1B).…”

Section: Introductionmentioning

confidence: 99%

“…Tri-O-benzyl-3-O-(2-naphthylmethyl)-d-mannonolactone(12):As olution of the hemiacetal 11 (742 mg, 1.26 mmol) in acetic anhydride (6.1 mL) and dry DMSO (6.6 mL) was stirred under N 2 for 22 h. The mixture was diluted with EtOAc (20 mL), quenched with ice and washed with water (3 20 mL) and brine (1 20 mL). The organic extracts were dried (MgSO 4 )a nd the solvent was evaporated.…”

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confidence: 99%

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Exploration of Strategies for Mechanism‐Based Inhibitor Design for Family GH99 endo‐α‐1,2‐Mannanases

Fernandes

Petricevic

Sobala

et al. 2018

Chemistry A European J

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endo‐α‐1,2‐Mannosidases and ‐mannanases, members of glycoside hydrolase family 99 (GH99), cleave α‐Glc/Man‐1,3‐α‐Man‐OR structures within mammalian N‐linked glycans and fungal α‐mannan, respectively. They are proposed to act through a two‐step mechanism involving a 1,2‐anhydrosugar “epoxide” intermediate incorporating two conserved catalytic carboxylates. In the first step, one carboxylate acts as a general base to deprotonate the 2‐hydroxy group adjacent to the fissile glycosidic bond, and the other provides general acid assistance to the departure of the aglycon. We report herein the synthesis of two inhibitors designed to interact with either the general base (α‐mannosyl‐1,3‐(2‐aminodeoxymannojirimycin), Man2NH2DMJ) or the general acid (α‐mannosyl‐1,3‐mannoimidazole, ManManIm). Modest affinities were observed for an endo‐α‐1,2‐mannanase from Bacteroides thetaiotaomicron. Structural studies revealed that Man2NH2DMJ binds like other iminosugar inhibitors, which suggests that the poor inhibition shown by this compound is not a result of a failure to achieve the expected interaction with the general base, but rather the reduction in basicity of the endocyclic nitrogen caused by introduction of a vicinal, protonated amine at C2. ManManIm binds with the imidazole headgroup distorted downwards, a result of an unfavourable interaction with a conserved active site tyrosine. This study has identified important limitations associated with mechanism‐inspired inhibitor design for GH99 enzymes.

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“…This process has little biological precedent (for a related proposal see Ref. ), but occurs in the base‐promoted solvolysis of α‐mannosides …”

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

mentioning

confidence: 99%

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Exploration of Strategies for Mechanism‐Based Inhibitor Design for Family GH99 endo‐α‐1,2‐Mannanases

Fernandes

Petricevic

Sobala

et al. 2018

Chemistry A European J

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“…[25] Due to the noveltyo fo ur chemistry, am echanistic study was necessitated. [25] Due to the noveltyo fo ur chemistry, am echanistic study was necessitated.…”

Section: Resultsmentioning

confidence: 99%

Synthesis of Nucleosides through Direct Glycosylation of Nucleobases with 5‐O‐Monoprotected or 5‐Modified Ribose: Improved Protocol, Scope, and Mechanism

Downey

Pohl

Roithová

et al. 2017

Chemistry A European J

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Simplifying access to synthetic nucleosides is of interest due to their widespread use as biochemical or anticancer and antiviral agents. Herein, a direct stereoselective method to access an expansive range of both natural and synthetic nucleosides up to a gram scale, through direct glycosylation of nucleobases with 5-O-tritylribose and other C5-modified ribose derivatives, is discussed in detail. The reaction proceeds through nucleophilic epoxide ring opening of an in situ formed 1,2-anhydrosugar (termed "anhydrose") under modified Mitsunobu reaction conditions. The scope of the reaction in the synthesis of diverse nucleosides and other 1-substituted riboside derivatives is described. In addition, a mechanistic insight into the formation of this key glycosyl donor intermediate is provided.

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“…8 Bennet et al reported computational analysis of formation of unprotected 1,2-anhdyro sugars from p-nitrophenyl glycosides. 9 Quite recently, the participation of a partially protected 1,2-anhydrofuranose was confirmed in a nucleoside synthesis. 10 However, in spite of the fact that unprotected 1,2-anhydro sugars possess potential utilities as a new donor substrate in the synthetic field of glycoscience, the direct experimental observation of totally unprotected 1,2-anhydro sugars has not been achieved yet.…”

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confidence: 97%

First Detection of Unprotected 1,2-Anhydro Aldopyranoses

Serizawa

Noguchi

et al. 2017

Chem. Lett.

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C2-Oxyanion Neighboring Group Participation: Transition State Structure for the Hydroxide-Promoted Hydrolysis of 4-Nitrophenyl α-d-Mannopyranoside

Cited by 32 publications

References 62 publications

Exploration of Strategies for Mechanism‐Based Inhibitor Design for Family GH99 endo‐α‐1,2‐Mannanases

Exploration of Strategies for Mechanism‐Based Inhibitor Design for Family GH99 endo‐α‐1,2‐Mannanases

Synthesis of Nucleosides through Direct Glycosylation of Nucleobases with 5‐O‐Monoprotected or 5‐Modified Ribose: Improved Protocol, Scope, and Mechanism

First Detection of Unprotected 1,2-Anhydro Aldopyranoses

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