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Stereoselective Total Synthesis of (±)‐Ptilocaulin and its 7‐Epimer. A Strategy Based On the Use of an Intramolecular Nitrile Oxide Olefin Cycloaddition (INOC) Reaction
Author(s) -
Keshava Murthy K.S.,
Hassner Alfred
Publication year - 1991
Publication title -
israel journal of chemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.908
H-Index - 54
eISSN - 1869-5868
pISSN - 0021-2148
DOI - 10.1002/ijch.199100028
Subject(s) - chemistry , intramolecular force , cycloaddition , stereoselectivity , nitrile , ketone , epimer , aldol condensation , guanidine , olefin fiber , stereocenter , substituent , medicinal chemistry , stereochemistry , organic chemistry , enantioselective synthesis , catalysis
A stereoselective total synthesis of (±)‐ptilocaulin 1 , an antimicrobial anticancer agent as well as of its 7‐epimer 23 is described. The strategy involves an aldol condensation of the dilithio dianion of the Z ‐aldoxime ( 13 ) with a ketone 6 to produce 11 and the stereospecific intramolecular cycloaddition of the nitrile oxide 5 , generated in situ from 11. The resulting isoxazoline 4 was converted to hydroxy ketone 3 which serves as a starting point for introduction of the fourth stereocenter at C‐7. Lithium in ethylamine reduction of 3 produces stereospecifically the 7β‐methyl compound which leads to ptilocaulin 1 , while catalytic hydrogenation of 3 introduces the 7α‐methyl substituent and finally 7‐epiptilocaulin 23. H‐ and C NMR analysis permits differentiation between isomers of intermediates. When, in the last step of the synthesis of 1 or 23 from 19 or 22 and guanidine, a higher temperature (>130 °C) was applied, an interesting disproportionation to aminopyrimidine 25 or 28 and cyclic guanidine 24 or 27 was observed.