What does this research mean for the field?

PEGylated 111In-radiolabeled albumin liposomes exhibit high stability and accumulate effectively in tumors via the enhanced permeability and retention effect, enabling long-term tumor imaging up to 96 hours. Novelty: ClaimNovelty.METHODOLOGICAL. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

The aim is to develop a radiopharmaceutical agent for long-term imaging of tumors in oncologic patients.

May 20, 2026

Development of radiolabeled 111In-albumin liposomes for long-term imaging of tumors.

Key Points

The aim is to develop a radiopharmaceutical agent for long-term imaging of tumors in oncologic patients.
Evaluation of biodistribution in C26-colon carcinoma tumor-bearing mice through radioactivity measurement and gamma scintigraphy imaging.
Analysis of the stability of PEGylated liposomes in serum and their accumulation in tumor sites.
Radiolabeled liposomes, sized approximately 130 nm, showed accumulation in tumor sites due to enhanced penetration and retention (EPR) (P<0.001).
High stability in maintaining encapsulated albumin for at least 96 hours with significant radioactivity detected in the kidneys, liver, spleen, and tumor regions.
Gamma scintigraphy imaging revealed organ hotspots indicating effective accumulation and stability in tumor sites over time.

Abstract

BACKGROUND: The current study aims to develop a clinically applicable radiopharmaceutical agent for long-term imaging in the diagnosis and management of oncologic patients in the field of nuclear medicine. Liposomes, as pharmaceutical nanocarriers, have been extensively studied in pharmaceutical industry and depending on their structural characteristics could be formulated for accumulation in various pathological sites in the body. PEGylated liposomes have smaller volume of distribution and decreased clearance, consequently, due to their more prolonged presence in the bloodstream and their stability during this time, could be used for tumor imaging. STUDY DESIGN AND METHODS: In-oxine and their stability in serum medium was assessed and the rate of their biodistribution in C26-colon carcinoma tumor-bearing mice was evaluated by two approaches, quantitatively radioactivity measurement and qualitatively gamma scintigraphy imaging. RESULTS: In -radiolabeled liposomes having a size of about 130 nanometers, were capable of accumulating in tumor sites based on enhanced penetration and retention (EPR) phenomenon. These liposomes also have high stability for maintaining encapsulated albumin for a long time up to 96 h and even may be stable for longer time period. In the study of biodistribution of our formulation in tumor-bearing mice, they accumulated more in the kidney, liver, spleen and tumor sites, so that even after clearance of formulation in the bloodstream, they existed in significantly higher levels in the mentioned organs and likewise tumor sites up to 96 h. In gamma scintigraphy, organs with high activity resulted from accumulation, were visible in the form of hot spots demonstrating formulation stability in the tumor sites from time of administration to 96 h. CONCLUSIONS: Our in vitro and in vivo studies demonstrated that this PEGylated radiolabeled liposomal formulation have considerable stability and efficiency for long-term tumor imaging which merit further studies for its transformation into clinical application.

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Development of radiolabeled 111In-albumin liposomes for long-term imaging of tumors.

Key Points

Abstract

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