AI Article Synopsis
- The study focused on regio- and stereoselective 1,3-dipolar cycloadditions involving C-(3-pyridyl)-N-phenylnitrone and various dipolarophiles to synthesize substituted pyridyl-isoxazolidines.
- A reductive cleavage method using ammonium formate and Pd/C effectively transformed these isoxazolidines into β- and β-amino alcohols, showing how substituents impact torsional angles.
- The methodology offers a safer and more cost-effective alternative to traditional hydrogenation methods, with theoretical support explaining the formation of amino-alcohols from bicyclic isoxazolidines.
Article Abstract
Regio- and stereoselective 1,3-dipolar cycloadditions of C-(3-pyridyl)-N-phenylnitrone (2) with variedly substituted dipolarophiles (3, 4) were carried out to obtain substituted pyridyl-isoxazolidines (5-8). Reductive cleavage of pyridyl-isoxazolidines (5-8) with ammonium formate, methanol-THF solvents, at ambient temperature, in the presence of Pd/C provided a facile route for the synthesis of β -and β -amino alcohols (9-12), with a substitution pattern having pronounced influence on torsional angles. The obtained compounds (9-12) are valuable scaffolds which can be utilized for peptidomimetics. Thus, the present methodology for reductive opening of isoxazolidine ring avoids the disadvantages of using expensive apparatus and hazards involved in the use of hydrogen gas. The preferential formation of amino-alcohols in case of bicyclic isoxazolidines (8a-c), which precludes any recyclization is rationalized by DFT calculations.
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| http://dx.doi.org/10.1002/cbdv.202301323 | DOI Listing |
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