Total Synthesis of Complanadine a

Brandon S Martin, Purdue University

Abstract

Described herein is the development of a total synthesis of the Lycopodium alkaloids lycodine and complanadine A. The Lycopodium alkaloids, particularly the lycodine-type, have generated broad interest in the scientific community due to their acetylcholinesterase inhibitory and other biological activity. Complanadine A is a particularly interesting target due to both its demonstrated ability to induce secretion of nerve growth factor in human glial cells, allowing observation of neurite outgrowth in rat neuronal PC-12 cells, and its structural complexity, being an unsymmetrical C1 − C2′ bipyridyl dimer of lycodine.Chapter 1 reviews the established routes for the synthesis of selected representative Lycopodium alkaloids, and Chapter 2 describes our efforts towards their total synthesis. The synthesis employs robust and underutilized methods for heterocycle construction, using a pyrrole intermediate for their unique nucleophilicity among aryl heterocycles. A pyrrole intermediate is converted in one step to a β-chloropyridine derivative via a Ciamician-Dennstedt reaction, with the halide serving as a convenient handle for elaboration of the lycodine scaffold to complanadine A via Fagnou coupling.

Degree

Ph.D.

Advisors

Dai, Purdue University.

Subject Area

Behavioral Sciences|Organic chemistry

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