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Studies on total synthesis of veratrum alkaloids Brookes, Roderick William

Abstract

The initial work toward a synthetic entry into the hexacyclic cevane nucleus (7) is described, and the specific application of this work to the total synthesis of verticine (12) is discussed. Hecogenin acetate (74) was converted to C-nor-D-homo-(25 R)-5α-spirost-13(18)-en-3β-ol-3-acetate (79) via a known procedure, and hydroboration of the double bond gave the corresponding 13β-hydroxymethyl compound (80(a)). The mass spectral fragmentation of the spiroketal system is discussed. The stereochemistry at C-13 of the hydroborated compound (80(a)) was reversed by oxidation of the primary alcohol to the aldehyde, epimerization, and reduction. Acetylation gave the diacetate (85) which was used in investigation of the spiroketal side chain degradation. The Baeyer-Villiger oxidation sequence developed by W.F. Johns was used in the spiroketal degradation. 13α-Acetoxymethyl-17-acetyl-18-nor-5α-etiojerv-16(17)-en-3β-ol-3-acetate (110) was obtained with considerable difficulty in low yield from this sequence, A model compound, 17-acetyl-5α, 13β-etiojerv-16(17)-en-3β-ol (111), was employed to test the feasibility of attachment of a heterocyclic portion via a reaction developed by Schreiber and Adam. Reduction of the double bond and epimerization of the methyl ketone gave the ketone (120), which was then condensed with 2-lithio-5-methylpyridine. The structure of the condensation product was established by its n.m.r. and mass spectra.

Item Metadata

Title
Studies on total synthesis of veratrum alkaloids
Creator
Brookes, Roderick William
Publisher
University of British Columbia
Date Issued
1969
Description
The initial work toward a synthetic entry into the hexacyclic cevane nucleus (7) is described, and the specific application of this work to the total synthesis of verticine (12) is discussed. Hecogenin acetate (74) was converted to C-nor-D-homo-(25 R)-5α-spirost-13(18)-en-3β-ol-3-acetate (79) via a known procedure, and hydroboration of the double bond gave the corresponding 13β-hydroxymethyl compound (80(a)). The mass spectral fragmentation of the spiroketal system is discussed. The stereochemistry at C-13 of the hydroborated compound (80(a)) was reversed by oxidation of the primary alcohol to the aldehyde, epimerization, and reduction. Acetylation gave the diacetate (85) which was used in investigation of the spiroketal side chain degradation. The Baeyer-Villiger oxidation sequence developed by W.F. Johns was used in the spiroketal degradation. 13α-Acetoxymethyl-17-acetyl-18-nor-5α-etiojerv-16(17)-en-3β-ol-3-acetate (110) was obtained with considerable difficulty in low yield from this sequence, A model compound, 17-acetyl-5α, 13β-etiojerv-16(17)-en-3β-ol (111), was employed to test the feasibility of attachment of a heterocyclic portion via a reaction developed by Schreiber and Adam. Reduction of the double bond and epimerization of the methyl ketone gave the ketone (120), which was then condensed with 2-lithio-5-methylpyridine. The structure of the condensation product was established by its n.m.r. and mass spectra.
Genre
Thesis/Dissertation
Type
Text
Language
eng
Date Available
2011-05-13
Provider
Vancouver : University of British Columbia Library
Rights
For non-commercial purposes only, such as research, private study and education. Additional conditions apply, see Terms of Use https://open.library.ubc.ca/terms_of_use.
DOI
10.14288/1.0060043
URI
http://hdl.handle.net/2429/34565
Degree
Master of Science - MSc
Program
Chemistry
Affiliation
Science, Faculty of; Chemistry, Department of
Degree Grantor
University of British Columbia
Campus
UBCV
Scholarly Level
Graduate
Aggregated Source Repository
DSpace

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For non-commercial purposes only, such as research, private study and education. Additional conditions apply, see Terms of Use https://open.library.ubc.ca/terms_of_use.