Enantioselective Syntheses of Conformationally Rigid,Highly Lipophilic Mesityl‐Substituted Amino Acids

Three N‐Boc‐protected amino acids substituted with a mesityl (=2,4,6‐trimethylphenyl) group were synthesized in enantiomerically pure form, either by asymmetric epoxidation or by aminohydroxylation as the source of chirality. The 3‐mesityloxirane‐2‐methanol 7 , easily available in high enantiomer purity by Sharpless epoxidation, was converted into 3‐{[(tert‐butoxy)carbonyl]amino}‐3‐mesitylpropane‐1,2‐diol 9 by a regio‐ and stereoselective ring opening with an ammonia equivalent (sodium azide or benzhydrylamine), followed by hydrogenation and in situ treatment with (Boc)₂O (Boc=[(tert‐butoxy)carbonyl]) (Scheme 3). Oxidative cleavage of the diol fragment in 9 afforded N‐[(tert‐butoxy)carbonyl]‐α‐mesitylglycine 1 of >99% ee. This amino acid was also prepared in enantiomerically pure form starting from 2,4,6‐trimethylstyrene ( 11 ) by a regioselective Sharpless asymmetric aminohydroxylation, followed by a 2,2,6,6‐tetramethylpiperidin‐1‐yloxyl (TEMPO)‐catalyzed oxidation (Scheme 4). On the other hand, 1‐[(tert‐butoxy)carbonyl]‐2‐{{[(tert‐butyl)dimethylsilyl]oxy}methyl}‐3‐mesitylaziridine 14 was prepared from 9 by a sequence involving selective protection of the primary alcohol (as a silyl ether), activation of the secondary alcohol as a mesylate, and base‐induced (NaH) cyclization (Scheme 5). The reductive cleavage of the aziridine ring (H₂, Pd/C), followed by alcohol deprotection (Bu₄NF/THF) and oxidation (pyridinium dichromate (PDC)/DMF or (TEMPO)/NaClO) provided, in high yield and enantiomeric purity, N‐[(tert‐butoxy)carbonyl]‐β‐mesitylalanine 2 . Alternatively, the regioselective ring opening of the aziridine ring of 14 with lithium dimethylcuprate, followed by silyl‐ether cleavage and oxidation lead to N‐[(tert‐butoxy)carbonyl]‐β‐mesityl‐β‐methylalanine 3 . A conformational study of the methyl esters of the N‐Boc‐protected amino acids 1 and 3 carried out by variable‐temperature ¹H‐NMR and semi‐empirical (AM1) calculations shows the strong rotational restriction imposed by the mesityl group.