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Tyrosine modified analogues of the 伪4尾7 integrin inhibitor biotin-R8ERY prepared via Click Chemistry: Synthesis and biological evaluation
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摘要
Our continuing programme aiming at developing inhibitors of integrin 伪4尾7, a key mediator of various inflammatory diseases, led us to synthesise a library of cell-permeable peptides based on the biotin-R8ERY鈭?/sup> template, wherein the tyrosine residue has been modified by using the CuAAC reaction. The peptidomimetics were evaluated in a cell adhesion assay and shown to inhibit Mn2+-activated adhesion of mouse TK-1 T cells to mouse MAdCAM-1. Two of the synthesised peptidomimetics, analogues 11 and 14, are more active than our previously reported lead compound biotin-r9YDRREY at concentrations of 100 and 50 渭M, with 14 exhibiting an IC50 of less than 10 渭M.

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