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Unlocking the potential of protein-derived peptides to target G-quadruplex DNA: from recognition to anticancer activity.


ABSTRACT: Noncanonical nucleic acid structures, particularly G-quadruplexes, have garnered significant attention as potential therapeutic targets in cancer treatment. Here, the recognition of G-quadruplex DNA by peptides derived from the Rap1 protein is explored, with the aim of developing novel peptide-based G-quadruplex ligands with enhanced selectivity and anticancer activity. Biophysical techniques were employed to assess the interaction of a peptide derived from the G-quadruplex-binding domain of the protein with various biologically relevant G-quadruplex structures. Through alanine scanning mutagenesis, key amino acids crucial for G-quadruplex recognition were identified, leading to the discovery of two peptides with improved G-quadruplex-binding properties. However, despite their in vitro efficacy, these peptides showed limited cell penetration and anticancer activity. To overcome this challenge, cell-penetrating peptide (CPP)-conjugated derivatives were designed, some of which exhibited significant cytotoxic effects on cancer cells. Interestingly, selected CPP-conjugated peptides exerted potent anticancer activity across various tumour types via a G-quadruplex-dependent mechanism. These findings underscore the potential of peptide-based G-quadruplex ligands in cancer therapy and pave the way for the development of novel therapeutic strategies targeting these DNA structures.

SUBMITTER: Merlino F 

PROVIDER: S-EPMC11229374 | biostudies-literature | 2024 Jul

REPOSITORIES: biostudies-literature

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Unlocking the potential of protein-derived peptides to target G-quadruplex DNA: from recognition to anticancer activity.

Merlino Francesco F   Marzano Simona S   Zizza Pasquale P   D'Aria Federica F   Grasso Nicola N   Carachino Alice A   Iachettini Sara S   Biroccio Annamaria A   Fonzo Silvia Di SD   Grieco Paolo P   Randazzo Antonio A   Amato Jussara J   Pagano Bruno B  

Nucleic acids research 20240701 12


Noncanonical nucleic acid structures, particularly G-quadruplexes, have garnered significant attention as potential therapeutic targets in cancer treatment. Here, the recognition of G-quadruplex DNA by peptides derived from the Rap1 protein is explored, with the aim of developing novel peptide-based G-quadruplex ligands with enhanced selectivity and anticancer activity. Biophysical techniques were employed to assess the interaction of a peptide derived from the G-quadruplex-binding domain of the  ...[more]

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