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Indole is one of the most important heterocycles widely present in bioactive natural products, pharmaceuticals, agrochemicals and materials. Being easily accessible, the 2-nitrostyrenes are attractive starting materials for the indole synthesis and the Cadogan-Sundberg reaction is one of the well-established methods exploiting the reductive cyclization of 2-nitrostyrene derivatives. The harsh reaction conditions associated with this named reaction [reflux in P(OEt)3] limited, nevertheless, its synthetic applications. Consequently, alternative conditions combining different transition metal catalysts with a terminal reductant have been developed. Recently, our group demonstrated that aqueous TiCl3 is a mild reductant capable of promoting the reductive cyclization of 2-nitrostyrene derivatives at room temperature leading to diversely substituted indoles or indolenines. The reaction was featured in the total synthesis of complex natural products such as (+)-1,2-dehydroaspidospermidine, (+)-condyfoline and (-)-tubifoline.This thesis focuses on the development of TiCl3-promoted reductive cyclization of previously unexploited substrates for the synthesis of important heterocycles and their applications in natural product synthesis. In chapter 2, we describe a novel synthesis of 3-acyloxy-2,3-disubstituted indolenines via TiCl3-mediated reductive cyclization of tetrasubstituted enol esters bearing a 2-nitrostyrene substituent. Mechanistically, a domino process involving a partial reduction of the nitro to nitroso group followed by a 5-center-6p-electrocyclization, 1,2-acyloxy migration and further reduction of the resulting nitrone intermediate accounts for the reaction outcome. This operationally simple reaction (aqueous TiCl3 solution, MeCN, 0 °C to room temperature) tolerates a wide range of functional groups affording 3-acyloxy-2,3-disubstituted indolenines in good to high yields. Conceptually, this important heterocycle is accessed for the first time under reductive conditions.Chapter 3 details our approach towards the total synthesis of trigonoliimine C, a pentacyclic bisindole alkaloid, featuring the reductive cyclization of enol esters as a key step. The requisite enol ester was synthesized via following a two steps procedure: a) Ketone synthesis via the Liebeskind-Srogl coupling; b) Enol ester formation by treatment of the ketone with LiHMDS at -78 °C followed by addition of Ts2O. However, all attempts to generate the 3-acyloxy-2,3-disubstituted indolenines met with failure at the present stage of development.Benzofuro[3,2-b]indoline is a key structural motif found in phalarine. It is synthetically much more difficult to access than its isomer, the benzofuro[2,3-b]indoline. The few existing methods suffer from the low regioselectivity in the oxidative coupling of two selected building blocks. We describe in Chapter 4 a TiCl3-mediated reductive cyclization of tetrasubstituted alkenes bearing a 2-nitrophenyl substituent and a properly tethered nucleophile. The starting materials were prepared via a key Suzuki-Miyaura cross couping of tosyl enol ester with aryl boronic acid based on Gosselin's report. Treatment of a MeCN solution of tetrasubstituted alkenes with aqueous TiCl3 and NH4OAc afforded the desired (benzo)furo[3,2-b]indolines in good to high yield with excellent regioselectivities. Total synthesis of phalarine featuring this novel reductive cyclization methodology was exploited and is being pursued in our laboratory.
Qian Wang, Jieping Zhu, Baochao Yang, Tristan Corentin Pierre Delcaillau
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