Synthesis of Fmoc-Protected trans-4-Methylproline

Synthesis of Fmoc-Protected trans-4-Methylproline

Fmoc-protected trans-4-methylproline was synthesized starting from d-serine. The chiral scaffold of serine in the form of olefinated Garner's aldehyde 3 was used to control the diastereoselective formation of the new stereocenter on the hydrogenation of allylic alcohol 4. The diastereoselectivi...

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Veröffentlicht in:Journal of organic chemistry 2001-03, Vol.66 (6), p.2061-2066
Hauptverfasser: Nevalainen, Marta, Kauppinen, Pasi M, Koskinen, Ari M. P
Format: Artikel
Sprache:eng
Schlagworte:
Amino Acids - chemistry
Fluorenes - chemistry
Magnetic Resonance Spectroscopy
Mass Spectrometry
Proline - analogs & derivatives
Proline - chemical synthesis
Proline - chemistry
Spectrum Analysis
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Zusammenfassung:Fmoc-protected trans-4-methylproline was synthesized starting from d-serine. The chiral scaffold of serine in the form of olefinated Garner's aldehyde 3 was used to control the diastereoselective formation of the new stereocenter on the hydrogenation of allylic alcohol 4. The diastereoselectivity (syn/anti ratio) of the process was 86:14, attained with Raney nickel. Hydrogen migration seems not to be the sole factor lowering the diastereoselectivity, as nickel is known not to promote double-bond migration. Instead, the moderate stereocontrol is attributed to the mobility of the side chain of 4, which allows the attack of hydrogen on both faces of the olefin (open transition state). A series of transformations led to ring precursor 8, which after recrystallization afforded the syn diastereoisomer in dr = 95:5. Protected trans-4-methylproline 11 was obtained from 8 in a straightforward fashion.
ISSN:0022-3263
1520-6904
DOI:10.1021/jo005726s