Si-Yen Liu et al., International Journal of Molecular Sciences 2021
Summary
Liposomes are often used in drug delivery due to their versatile structure, nontoxicity, and biodegradability. PEGylated liposomes can more effectively target radionuclides, pharmaceuticals to tumor cells due to their increased half-life within blood circulation, absorption, and lower toxicity.
As αVβ3 integrin is highly expressed on activated endothelium in malignant tissues, thus it is an effective angiogenic marker in the tumor progression. Additionally, this integrin subtype selectively binds to RGD peptides (extracellular matrix proteins, containing arginin-glycine-aspatic acid sequence). Incorporation of the RGD tripeptide into a cyclic pentapeptide has been found to increase binding affinity and selectivity for integrin αvβ3 receptor. Additionally, replacement of the 5th amino acid is also crucial since it enables further modifications (e.g., conjugation).
In this study, a radiolabeled 111In-cyclic RGDfK-liposome was prepared, molecular targeted imaging and efficacy of the nanoparticle for tumor imaging was evaluated.
The 111In-labeled-liposome or the 111In-labeled cyclic RGDfK-liposome was injected intravenously into the mice with human melanoma cells. They were scanned with nanoSPECT/CT PLUS 24h later. Results show that mice receiving the 111Inlabeled cyclic RGDfK-liposome showed high and specific tumor uptake. Based upon these findings, the cyclic RGDfK- liposome is said to be a promising agent for tumor imaging. Present study also reports successful design of modifying the surface of conventional liposome to add the cyclic RGDfK peptide for the targeted delivery of the radioactive cyclic RGDfK liposome to human melanoma cells, where the αVβ3 integrin was expressed.
Results from nanoSPECT/CT PLUS
Nude mice were injected subcutaneously with 2x105 A375.S2 human melanoma cells in their necks. Two weeks after the injection, animals had developed nodules of similar size, about 2 mm in diameter. For taking nuclear images with NanoSPECT/CT®plus scanner system, mice were injected with the 111In-labeled liposomes (50µCi), and the images of mice was captured 24 h after an injection of radioactive liposomes.
Results show that:
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