Efficient synthesis of terminal α,β-unsaturated ketones as the intermediates of the proteasome epoxyketone inhibitors via Weinreb

Abstract

Abstract:

Peptidyl epoxyketones were potential antitumor agents due to their 20S proteasome inhibitory activities. Based on their structures and special inhibitory mechanism, a series of compounds were designed by linking the epoxyketone moiety (the C-terminal pharmacophore) and the peptide backbones. To make these compounds, we used a novel method to prepare the terminal α,β-unsaturated ketone, the crucial intermediate, from Weinreb amide with satisfactory yield (62%–65%).

Key words: Epoxyketone, Epoxyketone, Synthesis, Synthesis, α,β-Unsaturated ketone, α,β-Unsaturated ketone, Weinreb amide, Weinreb amide

CLC Number:

R916.41

Supporting:

Yang Lü, Xiao-Min Zou, Ke Mou, Yi-Qiu Fu, Chao Ma, Bo Zhou, Ping Xu^*

Efficient synthesis of terminal α,β-unsaturated ketones as the intermediates of the proteasome epoxyketone inhibitors via Weinreb

[J]. .

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Efficient synthesis of terminal α,β-unsaturated ketones as the intermediates of the proteasome epoxyketone inhibitors via Weinreb

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