A "cross-stitched" peptide with improved helicity and proteolytic stability

一种“交叉缝合”肽,具有更高的螺旋性和蛋白水解稳定性

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Abstract

A new computational approach to obtain quantitative energy profiles for helix folding was used in the design of orthogonal hydrocarbon and lactam bicyclic peptides. The proteolytically stable, "cross-stitched" peptide SRC2-BCP1 shows nanomolar affinity for estrogen receptor α and X-ray crystallography confirms a helical binding pose.

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