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Scandium-44 Radiolabeled Peptide and Peptidomimetic Conjugates Targeting Neuropilin-1 Co-Receptor as Potential Tools for Cancer Diagnosis and Anti-Angiogenic Therapy

Autor
Gniazdowska, Ewa
Misicka-Kęsik, Aleksandra
Choiński, Jarosław
Walczak, Rafał
Tymecka, Dagmara
Witkowska, Ewa
Halik, Paweł Krzysztof
Redkiewicz, Patrycja
Masłowska, Katarzyna
Data publikacji
2023
Abstrakt (EN)

Pathological angiogenesis, resulting from an imbalance between anti- and pro-angiogenic factors, plays a pivotal role in tumor growth, development and metastasis. The inhibition of the angiogenesis process by the VEGF/VEGFR-2/NRP-1 pathway raises interest in the search for such interaction inhibitors for the purpose of the early diagnosis and treatment of angiogenesis-dependent diseases. In this work we designed and tested peptide-based radiocompounds that selectively bind to the neuropilin-1 co-receptor and prevent the formation of the pro-angiogenic VEGF-A165/NRP-1 complex. Three biomolecules, A7R and retro-inverso DR7A peptides, and the branched peptidomimetic Lys(hArg)-Dab-Pro-Arg (K4R), conjugated with macrocyclic chelator through two linkers’ types, were labeled with theranostic scandium-44 radionuclide, and studied in vitro as potential targeted radiopharmaceuticals. ELISA (enzyme-linked immunosorbent assay) studies showed no negative effect of the introduced biomolecules’ changes and high NRP-1 affinity in the case of A7R- and K4R-radiocompounds and a lack affinity for DR7A-radiocompounds. All radiopeptides showed a hydrophilic nature as well as high stability against ligand exchange reactions in cysteine/histidine solutions. Unfortunately, all radiocompounds showed unsatisfactory nano-scale stability in human serum, especially for use as therapeutic radioagents. Further work is ongoing and focused on the search for angiogenesis inhibitors that are more human serum stable.

Słowa kluczowe EN
angiogenesis
theranostic 43,44,47Sc-radiopharmaceuticals
anti-angiogenic therapy
neuropilin-1
VEGF-A165/NRP-1 complex inhibitor
angiogenic factors
A7R peptide
retro-inverso isomer DR7A
peptidomimetics
Dyscyplina PBN
nauki fizyczne
Czasopismo
Biomedicines
Tom
11
Zeszyt
2
Strony od-do
564
Data udostępnienia w otwartym dostępie
2023-02-15
Licencja otwartego dostępu
Uznanie autorstwa