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Controlling oncogenic KRAS signaling pathways with a Palladium-responsive peptide

Chemistry

Controlling oncogenic KRAS signaling pathways with a Palladium-responsive peptide

S. Learte-aymamí, P. Martin-malpartida, et al.

This exciting research showcases a bis-histidine peptide derived from the αH helix of the cofactor SOS1, which achieves high-affinity binding to KRAS when paired with Pd(II). The reversible binding turns it into a switchable KRAS binder, inhibiting the MAPK kinase cascade effectively. This is a breakthrough by the authors, highlighting the peptide's potential in cellular applications.... show more
Abstract
RAS oncoproteins are molecular switches associated with critical signaling pathways that regulate cell proliferation and differentiation. Mutations in the RAS family, mainly in the KRAS isoform, are responsible for some of the deadliest cancers, which has made this protein a major target in biomedical research. Here we demonstrate that a designed bis-histidine peptide derived from the αH helix of the cofactor SOS1 binds to KRAS with high affinity upon coordination to Pd(II). NMR spectroscopy and MD studies demonstrate that Pd(II) has a nucleating effect that facilitates the access to the bioactive α-helical conformation. The binding can be suppressed by an external metal chelator and recovered again by the addition of more Pd(II), making this system the first switchable KRAS binder, and demonstrates that folding-upon-binding mechanisms can operate in metal-nucleated peptides. In vitro experiments show that the metallopeptide can efficiently internalize into living cells and inhibit the MAPK kinase cascade.
Publisher
Communications Chemistry
Published On
Jun 23, 2022
Authors
Soraya Learte-Aymamí, Pau Martin-Malpartida, Lorena Roldán-Martín, Giuseppe Sciortino, José R. Couceiro, Jean-Didier Maréchal, Maria J. Macias, José L. Mascareñas, M. Eugenio Vázquez
Tags
bis-histidine peptide
KRAS binding
Pd(II) coordination
NMR spectroscopy
metallopeptide
MAPK kinase cascade
cellular internalization
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