3613-86-3

Upstream product

• 18779-77-6 scyllo-inosamine hexaacetate 
• 19046-72-1 penta-O-acetyl-2-acetylamino-2-deoxy-myo-inositol 
• 80681-52-3 C₂₆H₄₅NO₂₀ 
• 77101-18-9 C₃₂H₅₅NO₂₄ 
• 80681-50-1 C₃₀H₅₁NO₂₅ 
• 4969-30-6 (2R,3R,4S,6R)-6-Nitro-cyclohexane-1,2,3,4,5-pentaol 
• 6556-12-3 D-glucuronic acid 
• 108-24-7 acetic anhydride 
• 488-53-9 (2R,3R,4S,6R)-6-Amino-cyclohexane-1,2,3,4,5-pentaol 
• 7045-48-9 myo-inosose-⁽²⁾-phenylhydrazone 
• 2772-86-3 DL-penta-O-acetyl-2-acetylamino-2-deoxy-epi-inositol 
• 16051-25-5 1-amino-1-deoxy-scyllo-inositol 
• 527-22-0 6c-amino-cyclohexane-1r,2t,3c,4t,5c-pentaol 
• 251538-17-7 (1S,2R,3S,6R)-6-azido-2-bromocyclohex-4-ene-1,3-diol 

Downstream Products

• 20097-49-8 penta-O-acetyl-3-acetylamino-3-deoxy-muco-inositol 
• 64938-54-1 1D-penta-O-acetyl-1-acetylamino-1-deoxy-myo-inositol 
• 7011-06-5 penta-O-acetyl-1-acetylamino-1-deoxy-scyllo-inositol 

Relevant academic research and scientific papers

A Chiron Approach to Diversity-Oriented Synthesis of Aminocyclitols, (-)-Conduramine F-4 and Polyhydroxyaminoazepanes from a Common Precursor

The total syntheses of aminocyclitols, (-)-conduramine F-4, and polyhydroxyaminoazepanes have been achieved from a common precursor derived from tri-O-benzyl-d-glucal through a 'diversity-oriented' approach. Tri-O-benzyl-d-glucal was converted into a protected 1,6-diol through a sequence of steps that include transformation to a 2-tosylamidoglucose derivative, selective deprotection of primary C-6 benzyloxy group, LiAlH4-mediated one-step reduction of acetate groups, and reductive ring opening of the resulting hemiacetal as the key steps. The 1,6-diol served as a common precursor in our diversity oriented approach toward the target molecules. Mesylation of the diol followed by double nucleophilic substitution reaction with primary amines led to the synthesis of amino-substituted polyhydroxyazepanes. On the other hand, dialdehyde obtained from the oxidation of 1,6-diol was found to be a convenient starting material for the synthesis of aminocyclitols and (-)-conduramine F-4. McMurry coupling of the dialdehyde was successfully employed, for the first time, to construct the carbocyclic framework of aminoyclitols, while bis-Wittig olefination of the dialdehyde followed by Grubb's(II)-catalyzed RCM delivered (-)-conduramine F-4. The stereochemistry of newly created chiral centers in aminocyclitols was established through single crystal X-ray crystallography and detailed NOE studies.

Stereoselective synthesis of several azido/amino- and diazido/diamino-myo-inositols and their phosphates from p-benzoquinone

A practical route is described for the preparation of azido-myo-inositols, amino-myo-inositols and azido-conduritol B derivatives. Starting from p-benzoquinone, optically pure compounds in both forms can be prepared via enzymatic resolution of a derived diacetoxy conduritol B derivative. Selective introduction of nitrogen-containing functional groups in four of the six possible positions in the cyclitol moiety is followed by further functionalization to yield the target compounds.