Solid-phase total synthesis of trunkamide A(1)

Marine organisms are a rich source of novel, biologically active compounds. Herein, the solid-phase total synthesis of trunkamide A, currently in preclinical trials, is presented. Trunkamide A contains a thiazoline heterocycle and two residues of Ser and Thr with the hydroxy function modified as rev...

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Bibliographic Details
Published in:Journal of organic chemistry 2001-11, Vol.66 (23), p.7568-7574
Main Authors: Caba, J M, Rodriguez, I M, Manzanares, I, Giralt, E, Albericio, F
Format: Article
Language:English
Subjects:
Animals
Antineoplastic Agents - chemical synthesis
Peptides, Cyclic - chemical synthesis
Urochordata - chemistry
Online Access:Get full text
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Summary:Marine organisms are a rich source of novel, biologically active compounds. Herein, the solid-phase total synthesis of trunkamide A, currently in preclinical trials, is presented. Trunkamide A contains a thiazoline heterocycle and two residues of Ser and Thr with the hydroxy function modified as reverse prenyl (rPr). Cornerstones of the synthesis are as follows: (i) solid-phase peptide chain elongation using a quasi-orthogonal protecting scheme with tert-butyl and fluorenyl based groups, on a chlorotrityl resin; (ii) concourse of HOAt-based coupling reagents; and (iii) cyclizations in solution. Furthermore, the following synthetic steps are discussed: (i) preparation of the reverse prenyl derivatives of Ser and Thr; (ii) introduction of precursor of thiazoline as a protected amino thionoacid derivative; and (iii) formation of the thiazoline ring with DAST. All these features make this strategy particularly suitable for the large-scale synthesis of trunkamide A and other peptides containing the same motifs.
ISSN:0022-3263
DOI:10.1021/jo015703t