Synthesis and Structural Model of an α(2,6)‐Sialyl‐T Glycosylated MUC1 Eicosapeptide under Physiological Conditions
- 16 June 2006
- journal article
- research article
- Published by Wiley in Chemistry – A European Journal
- Vol. 12 (19) , 4981-4993
- https://doi.org/10.1002/chem.200600144
Abstract
To study the effect of O‐glycosylation on the conformational propensities of a peptide backbone, a 20‐residue peptide (GSTAPPAHGVTSAPDTRPAP) representing the full length tandem repeat sequence of the human mucin MUC1 and its analogue glycosylated with the (2,6)‐sialyl‐T antigen on Thr11, were prepared and investigated by NMR and molecular modeling. The peptides contain both the GVTSAP sequence, which is an effective substrate for GalNAc transferases, and the PDTRP fragment, a known epitope recognized by several anti‐MUC1 monoclonal antibodies. It has been shown that glycosylation of threonine in the GVTSAP sequence is a prerequisite for subsequent glycosylation of the serine at GVTSAP. Furthermore, carbohydrates serve as additional epitopes for MUC1 antibodies. Investigation of the solution structure of the sialyl‐T glycoeicosapeptide in a H2O/D2O mixture (9:1) under physiological conditions (25 °C and pH 6.5) revealed that the attachment of the saccharide side‐chain affects the conformational equilibrium of the peptide backbone near the glycosylated Thr11 residue. For the GVTSA region, an extended, rod‐like secondary structure was found by restrained molecular dynamics simulation. The APDTR region formed a turn structure which is more flexibly organized. Taken together, the joined sequence GVTSAPDTR represents the largest structural model of MUC1 derived glycopeptides analyzed so far.Keywords
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