An Intracellular Helix-constrained Peptide Library Screening Platform to Derive Functional Transcription Factor Antagonists
Description preview
>60% of all multi-protein complexes feature helical interfaces, with >20% participating in gene regulation. Helical interaction inhibitors therefore have enormous potential to become a useful class of transcriptional modulator. Small molecules typically fail to abrogate these interactions owing to their limited ability to extend beyond…
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