2026-04-17T06:08:28Zhttps://recercat.cat/oai/requestoai:recercat.cat:2445/1213142025-12-04T19:32:19Zcom_2072_1057col_2072_478908col_2072_478917col_2072_478933
RECERCAT
author
Guardiola Bagán, Salvador
author
Seco Moral, Jesús
author
Varese, Monica
author
Díaz Lobo, Mireia
author
García Arroyo, Jesús
author
Teixidó Turà, Meritxell
author
Nevola, Laura
author
Giralt Lledó, Ernest
2018-04-05T12:40:02Z2018-11-06T06:10:20Z2017-11-062018-04-05T12:40:02Z
In cancer, proliferation of malignant cells is driven by overactivation of growth-signalling mechanisms, such as the epidermal growth factor receptor (EGFR) pathway. Despite its therapeutic relevance, the EGF-EGFR interaction has remained elusive to inhibition by synthetic molecules, mostly as a result of its large size and lack of binding pockets and cavities. Designed peptides, featuring cyclic motifs and other structural constraints, have the potential to modulate such challenging protein-protein interactions (PPIs). Herein, we present the structure-based design of a series of bicyclic constrained peptides that mimic an interface domain of EGFR and inhibit the EGF-EGFR interaction by targeting the smaller partner (i.e., EGF). This design process was guided by the integrated use of in silico methods and biophysical techniques, such as NMR spectroscopy and surface acoustic wave. The best analogues were able to reduce selectively the viability of EGFR+ human cancer cells. In addition to their efficacy, these bicyclic peptides are endowed with exceptional stability and metabolic resistance-two features that make them suitable candidates for in vivo applications.
(c) Wiley-VCH, 2018 info:eu-repo/semantics/openAccess
Càncer
Pèptids
Proteïnes
Cancer
Peptides
Proteins
Toward a novel drug to target the EGF-EGFR interaction: design of metabolically stable bicyclic peptides
info:eu-repo/semantics/article info:eu-repo/semantics/acceptedVersion