Kenneth S. Feldman

Organic Synthesis

Professor Feldman's research interests span several areas of organic synthesis. One part of his program emphasizes the total synthesis of natural product target molecules, both as a testing ground for the development of new methodology for stereoselective construction of complex functional arrays and as a source of probe molecules to explore interactions with biological receptors. Another focus of the Feldman group is exploratory methodology development based on the interactions of reactive carbenes with proximate functionality. The goal of these studies is to devise efficient transformations for rapid assembly of polyheterocyclic target molecules. These projects rely on all of the intellectual and experimental advances of contemporary organic synthesis and offer a wide range of opportunities for inquiry.

One of the natural products projects explores the synthesis chemistry and immunomodulatory activity of a class of secondary plant metabolites called ellagitannins, exemplified by the dimer coriariin A (1). Several structural features of these compounds pose difficult challenges for organic synthesis, including the diastereoselective (atrop-selective) coupling of aromatic rings and the regioselective construction of diaryl ethers in polyphenolic substrates. We are developing novel solutions to these problems, and their application in ellagitannin synthesis has recently resulted in the preparation of coriariin A as well as several structural analogues. Recent in-house assays with human immune system cells demonstrated that coriariin A and related analogues can either upregulate secretion of tumor necrosis factor alpha (TNFa) or, alternatively, suppress its lipopolysaccharide (LPS, a bacterial toxin)-stimulated release, depending on the structural details of the tannin construct tested (Figs. 1 and 2). Enhanced release of TNFa presumably underlies the remarkable in vivo antitumor activity of coriariin A, while systemic overproduction of this cytokine stimulated by the bacterial toxin LPS can result in the often fatal condition septic shock. We are actively probing the mechanism by which these tannin species either agonize or antagonize LPS activity in an effort to develop a molecular-level understanding of the functional, structural and stereochemical requirements for biological activity. Companion studies designed to identify tannin analogs that can either 1) be targeted specifically to tumors, or 2) antagonize LPS activity with greater potency, are ongoing as well.

A second synthesis project is based on the facile generation of reactive alkylidene carbene intermediates 3 from combination of select nucleophiles with alkynyliodonium salts 2 (Fig. 3). These carbene intermediates participate in a range of subsequent intramolecular transformations, including C-H insertion, alkene cycloaddition, heteroatom (lone pair) addition, and arene addition/expansion, to furnish carbocyclic and heterocyclic products related to various families of alkaloids. The antileukemic alkaloids deoxyharringtonine (4) and pareitropone (5), the cytotoxic marine principle agelastatin A (6), and the selective VCAM-1 induction inhibitor halichlorine (7) are current synthesis targets of this chemistry.