330801-38-2

Upstream product

• 867-13-0 diethoxyphosphoryl-acetic acid ethyl ester 
• 122-78-1 phenylacetaldehyde 
• 330801-21-3 ethyl 2,2-difluoro-3-hydroxy-4-phenylbutanoate 
• 330801-32-6 N-(4-methoxyphenyl)-3-benzyl-2,2-difluoropropano-3-lactam 
• 330801-36-0 methyl 3-[N-(tert-butoxycarbonl)amino]-2,2-difluoro-4-phenylbutanoate 
• 330801-34-8 methyl 2,2-difluoro-3-[N-(4-methoxyphenyl)amino]-4-phenylbutanoate 
• 330801-30-4 N-(4-methoxyphenyl)-2,2-difluoro-3-hydroxy-4-phenylbutanamide 

Relevant academic research and scientific papers

SmI2-Mediated Reduction of γ,γ-Difluoro-α ,β-enoates with Application to the Synthesis of Functionalized (Z)-Fluoroalkene-Type Dipeptide Isosteres

A samarium diiodide (SmI2)-mediated reduction of γ,γ-difluoro-α,β-enoates (15, 29, and 34) was successfully applied to the synthesis of (Z)-fluoroalkene dipeptide isosteres (23, 30, and 35), which have served as potential dipeptide mimetics. Reduction of the γ,γ-difluoro-α,β-enoates by SmI2 proceeded via successive two-electron transfers to form dienolate species which upon kinetically controlled trapping with t-BuOH yielded Xaa-Gly-type fluoroalkene isosteres exemplified by 23, 30, and 35. Replacement of the t-BuOH kinetic trapping agent with aldehydes or ketones provided access to α-substituted fluoroalkene isosteres (43 and 45) through aldol reactions of Sm-dienolates with the carbonyl compounds. Of particular note, the use of the SmI2-HCHO reagent system with chiral enoate 34 provided D-Phe-ψ [(Z)-CF=CH]-D/L-Ser isosteres (45), which could be converted to enantiomerically pure isosteres (49-52) that bore a variety of side chain functionalities at the α-position. This was achieved by a sequence of manipulations consisting of β-lactone formation followed by chromatographic separation and ring-opening with soft nucleophiles. Included in the present work is the first utilization of a Rh-catalyzed Reformatsky reaction of chiral imines for the stereoselective preparation of α,α-difluoro-β-amino acid derivatives (28 and 33). The appropriate choice of reagents (carbonyl compounds for kinetic trapping or ring-opening nucleophiles and imines for Reformatsky reactions) allows the presented methodology to yield various fluoroalkene isosteres possessing a wide range of side chain functionalities.

Synthesis of (Z)-fluoroalkene dipeptide isosteres utilizing organocopper-mediated reduction of γ,γ-difluoro-α,β-enoates

γ,γ-Difluoro-α,β-enoates are reduced with organocopper reagents to afford the corresponding γ-fluoro-β,γ-enoates. This organocopper-mediated reduction was applied to the synthesis of (Z)-fluoroalkene dipeptide isosteres.