New Protecting Groups for the Synthesis of Complex Peptides

  1. Isidro Llobet, Albert
unter der Leitung von:
  1. Mercedes Álvarez Domingo Doktorvater/Doktormutter
  2. Fernando Albericio Palomera Doktorvater/Doktormutter

Universität der Verteidigung: Universitat de Barcelona

Fecha de defensa: 13 von Mai von 2008

Gericht:
  1. Antoni Riera Escalé Präsident/in
  2. Paul Lloyd-Williams Sekretär/in
  3. Andrés Parra Guerrero Vocal
  4. Juan José Vaquero López Vocal
  5. Eduard Bardají Rodríguez Vocal

Art: Dissertation

Teseo: 234021 DIALNET lock_openTDX editor

Zusammenfassung

The increasing importance of peptides as drugs creates the necessity of new methodologies for the synthesis of complex peptides. This PhD thesis has been focused on the development of new protecting groups (including new linkers) for peptide synthesis. The work done has solved several problems in peptide synthesis making it more versatile. These are some of the results obtained:- The removal conditions of the pNZ group as α-amino and Orn and Lys side chain protector have been optimized. These optimized conditions make pNZ orthogonal to the most used protecting groups in the Fmoc/tBu solid phase peptide synthesis strategy (Fmoc, Boc and Alloc) and minimize its most important side reactions such as formation of diketopiperazines, aspartimides and removal of the α-Fmoc group. The use of the pNZ group allows also the synthesis of complex and biologically interesting peptides such as the antitumoral peptide Kahalalide F.- A new protecting agent, the Fmoc-2-mercaptobenzothiazole (Fmoc-MBT), has been developed. It prevents side reactions in the synthesis of Fmoc-amino acids.New protecting groups developed:- p-Nitromandelic linker (pNM): it is useful for the synthesis of peptides and depsipeptides using the Boc/Bn strategy.- Backbone protectors (3,4-ethylenedioxythenyl (EDOTn) and 1-methyl-3-indolylmethyl (MIM)): they improve some of the poperties of the present backbone protectors such as their difficult elimination and steric hindrance.- Phenyl-EDOTn derivatives as super acid labile carboxylic acid protecting groups.- 1,2-dimethylindole-3-sulfonyl (MIS) as a protector of the side chain of arginine: it is much more acid labile than the present protecting groups and it is compatible with tryptophan containing peptides.