The first total synthesis of the cytotoxic marine metabolite agelastatin A (1) has been achieved in
about 14 steps performed in 12 operations in approximately 7% overall yield starting from cyclopentadiene.
Hetero Diels−Alder cycloaddition of cyclopentadiene with N-sulfinyl methyl carbamate (7) afforded cycloadduct
8, which without purification was converted to allylic sulfoxide 9 and then by a [2,3]-sigmatropic rearrangement
into bicyclic oxazolidinone 11. The C-5a nitrogen was introduced into the oxazolidinone Boc derivative 16 by
a Sharpless/Kresze allylic amination with SES sulfodiimide 12c. Palladium-promoted cyclization of 2-acyl
pyrroles 20 and 21 via a π-allylpalladium intermediate 22 led to ABC-tricycles 23 and 24, respectively. A
hydroxyl urea D-ring model system was constructed by hydroborating 24, leading eventually to keto amide 31
and then to tetracycle 33. A modified strategy was developed for synthesis of the pivotal tricyclic ketone 58,
involving as key steps a chemoselective hydrolysis of N-Boc oxazolidinone 54 and an internal conjugate addition
of pyrrolo cyclopentenone 57. A TMS group was used as a convenient substitute for the C-1 bromine substituent
of agelastatin A, and thus silylpyrrole 58 could be converted to bromopyrrole 59. Finally, the D-ring could be
annulated onto an α-amino ketone derived from 59 using methyl isocycanate, providing racemic agelastatin A
(1).
A catalytic antibody-based approach toward the synthesis of an optically active pyrrolidine ring synthon potentially useful for ptilomycalin A is described. Enantiomerically pure hapten 37 was designed and constructed with the eventual goal of generating antibodies for the enantioselective partial hydrolysis of a meso diester such as 44 into a monoacid 45. This transition state analog possesses a phosphonate group containing the requisite oxyanionic character of the tetrahedral intermediate for ester hydrolysis. A newly developed carbamate-based linker, which was found to be much more hydrolytically stable than the commonly used glutarate ester, was developed for coupling of the hapten to a carrier protein.
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