Macrocyclic RGD-peptides with high selectivity for αvβ3 integrin in cancer imaging and therapy

Abstract

Integrins, particularly the αvβ3 subtype, are critical receptors involved in cell adhesion, migration, and signaling, playing a significant role in tumor progression and metastasis. Despite extensive research into integrin-targeted therapies, challenges remain in developing ligands that exhibit high selectivity for αvβ3 over other integrin subtypes, such as αvβ5. This study employs a one-pot sortase A-mediated on-resin peptide cleavage and in situ cyclization method to synthesize two generations of macrocyclic RGD-peptide libraries. Systematic screening through surface plasmon resonance and cell-based competition assays identified the lead compound, c-(G5RGDKcLPET), which demonstrated high affinity and selectivity for αvβ3. Additionally, the optimized cyclic peptide was functionalized with a fluorescent dye (Cy5) and the cytotoxic drug monomethyl auristatin E (MMAE), enhancing its potential for cancer imaging and targeted therapy. This work contributes a novel platform for developing integrin-targeted diagnostics and therapeutics, highlighting the importance of macrocyclic peptides in cancer treatment strategies.

Graphical abstract: Macrocyclic RGD-peptides with high selectivity for αvβ3 integrin in cancer imaging and therapy

Supplementary files

Article information

Article type
Research Article
Submitted
02 Apr 2025
Accepted
27 Apr 2025
First published
03 May 2025

RSC Med. Chem., 2025, Advance Article

Macrocyclic RGD-peptides with high selectivity for αvβ3 integrin in cancer imaging and therapy

X. Cheng, C. Li, H. Hong, Z. Zhou and Z. Wu, RSC Med. Chem., 2025, Advance Article , DOI: 10.1039/D5MD00280J

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