A Lipopeptidomimetic of Transcriptional Activation Domains Selectively Disrupts the Coactivator Med25 Protein-Protein Interactions.
Olivia N PattelliEstefanía Martínez ValdiviaMatthew S BeyersdorfClint S ReganMónica RivasKatherine A HebertSofia D MerajverTomasz CierpickiAnna K MappPublished in: Angewandte Chemie (International ed. in English) (2024)
Short amphipathic peptides are capable of binding to transcriptional coactivators, often targeting the same binding surfaces as native transcriptional activation domains. However, they do so with modest affinity and generally poor selectivity, limiting their utility as synthetic modulators. Here we show that incorporation of a medium-chain, branched fatty acid to the N-terminus of one such heptameric lipopeptidomimetic (LPPM-8) increases the affinity for the coactivator Med25 >20-fold (Ki >100 μM to 4 μM), rendering it an effective inhibitor of Med25 protein-protein interactions (PPIs). The lipid structure, the peptide sequence, and the C-terminal functionalization of the lipopeptidomimetic each influence the structural propensity of LPPM-8 and its effectiveness as an inhibitor. LPPM-8 engages Med25 through interaction with the H2 face of its activator interaction domain and in doing so stabilizes full-length protein in the cellular proteome. Further, genes regulated by Med25-activator PPIs are inhibited in a cell model of triple-negative breast cancer. Thus, LPPM-8 is a useful tool for studying Med25 and mediator complex biology and the results indicate that lipopeptidomimetics may be a robust source of inhibitors for activator-coactivator complexes.
Keyphrases
- fatty acid
- gene expression
- transcription factor
- nuclear factor
- randomized controlled trial
- amino acid
- small molecule
- single cell
- genome wide
- dna methylation
- cystic fibrosis
- immune response
- stem cells
- lymph node
- cancer therapy
- bone marrow
- mesenchymal stem cells
- rectal cancer
- staphylococcus aureus
- pseudomonas aeruginosa
- genome wide analysis