Synthesis of Stable Cholesteryl–Polyethylene Glycol–Peptide Conjugates with Non-Disperse Polyethylene Glycol Lengths
A method for conjugating cholesterol to peptide ligands through non-disperse polyethylene glycol (ND-PEG) through a non-hydrolysable linkage is described. The iterative addition of tetraethylene glycol macrocyclic sulfate to cholesterol (Chol) renders a family of highly pure well-defined Chol-PEG compounds with different PEG lengths from 4 up to 20 ethylene oxide units, stably linked through an ether bond. The conjugation of these Chol-PEG compounds to the cyclic (RGDfK) peptide though Lys5 side chains generates different lengths of Chol-PEG-RGD conjugates that retain the oligomer purity of the precursors, as analysis by HRMS and NMR has shown. Other derivatives were synthesized with similar results, such as Chol-PEG-OCH3 and Chol-PEG conjugated to glutathione and Tf1 peptides through maleimide–thiol chemoselective ligation. This method allows the systematic synthesis of highly pure uniform stable Chol-PEGs, circumventing the use of activation groups on each elongation step and thus reducing the number of synthesis steps.
Auteurs principaux: | Cristóbal-Lecina, Edgar, Pulido, Daniel, Martin-Malpartida, Pau, Macías, María J., Albericio, Fernando, Royo, Miriam |
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Autres auteurs: | European Commission |
Format: | artículo biblioteca |
Langue: | English |
Publié: |
American Chemical Society
2020-03-06
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Sujets: | Cholesterol, Polyethylene, |
Accès en ligne: | http://hdl.handle.net/10261/207184 http://dx.doi.org/10.13039/501100000780 |
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