Synthesis of macrocyclic peptidomimetics: Via the Ugi-click-strategy

The Ugi-click-strategy was employed for the synthesis of 12-28 membered 1,2,3-triazole derived macrocyclic peptidomimetics. The Ugi reaction with acid components bearing acetylenic fragments and azidoisocyanides provided the corresponding peptidomimetics in up to 97% isolated yield. The subsequent CuAAC click reaction with these bifunctional substrates containing both acetylene and azide groups was investigated to reveal the influence of the structure of Ugi products on the direction of the click-cyclization. It was demonstrated that this approach allows efficient synthesis of either monomeric (12- and 13-membered) or dimeric (24-, 26- and 28-membered) macrocycles prepared in up to 85% yield. The scope and limitations of this method are discussed. © 2019 The Royal Society of Chemistry.

Authors
Zakharova E.A.1 , Shmatova O.I. 1 , Kutovaya I.V.1 , Khrustalev V.N. 2, 3 , Nenajdenko V.G. 1
Publisher
Royal Society of Chemistry
Number of issue
13
Language
English
Pages
3433-3445
Status
Published
Volume
17
Year
2019
Organizations
  • 1 Department of Chemistry, Lomonosov Moscow State University, Moscow, 119991, Russian Federation
  • 2 Peoples' Friendship University of Russia (RUDN University), 6 Miklukho-Maklay Street, Moscow, 117198, Russian Federation
  • 3 National Research Center, Kurchatov Institute, 1 Kurchatov Sq., Moscow, 123182, Russian Federation
Keywords
Chemistry; Positive ions; Bi-functional; Click reaction; Efficient synthesis; Isolated yield; Macrocycles; Macrocyclic peptidomimetics; Peptidomimetics; Ugi reaction; Cyclization
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