Synthesis of Piperazic Acid‐Containing Cyclodepsipeptide Core of Verucopeptin

Author:

Sun Yuanjun1,Tang Wenhao1,Wang Mei1,Ni Huxin1,Long Ya‐Qiu1

Affiliation:

1. Laboratory of Medicinal Chemical Biology, College of Pharmaceutical Sciences, Jiangsu Province Engineering Research Center of Precision Diagnostics and Therapeutics Development Soochow University Suzhou Jiangsu 215123 China

Abstract

Comprehensive SummaryChemically, N1 nitrogen of piperazic acid is more nucleophilic than N2 nitrogen, but amide bonds predominantly formed at N2 nitrogen are prevalent in piperazic acid‐containing natural products, with only one exception of sanglifehrin. Thus two orthogonal protecting groups of nitrogen are often employed to realize selective coupling of N2 nitrogen, resulting in increased synthetic steps and low synthetic efficiency. However, we develop selective deprotection of N2‐Cbz from the N1,N2‐diCbz‐piperazic acid‐containing peptide to form the N2 amide exclusively, avoiding the tedious orthogonal protection strategy which is commonly applied when the easily‐accessible N1,N2‐diCbz‐piperazic acid is used as the synthetic module. We employ this selective‐deprotection strategy to achieve an efficient synthesis of piperazic acid‐containing cyclodepsipeptide core of verucopeptin with an overall yield of 21% from commercially/readily available building blocks. The key steps include late stage coupling of piperazic acid with 3‐hydroxyleucine derivatives, and HATU‐mediated macrolactamization of 19‐membered macrocycle at N9 and C10. The selective deprotection of N2‐Cbz from the N1,N2‐diCbz‐piperazic acid at late‐stage would greatly facilitate the total syntheses of piperazic acid‐containing cyclodepsipeptides of biological interest.

Funder

China Postdoctoral Science Foundation

National Natural Science Foundation of China

Publisher

Wiley

Subject

General Chemistry

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