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Merck

Targeting of liposomes via PSGL1 for enhanced tumor accumulation.

Pharmaceutical research (2012-09-21)
Robert Carlisle, Leonard W Seymour, Constantin C Coussios
摘要

To improve the delivery of liposomes to tumors using P-selectin glycoprotein ligand 1 (PSGL1) mediated binding to selectin molecules, which are upregulated on tumorassociated endothelium. PSGL1 was orientated and presented on the surface of liposomes to achieve optimal selectin binding using a novel streptavidin-protein G linker molecule. Loading of PSGL1 liposomes with luciferin allowed their binding to e-selectin and activated HUVEC to be quantified in vitro and their stability, pharmacokinetics and tumor accumulation to be tested in vivo using murine models. PSGL1 liposomes showed 5-fold (p < 0.05) greater selectin binding than identically formulated control liposomes modified with ligand that did not contain the selectin binding domain. When added to HUVEC, PSGL1 liposomes showed >7-fold (p < 0.001) greater attachment than control liposomes. In in vivo studies PSGL1 liposomes showed similar stability and circulation to control liposomes but demonstrated a >3-fold enhancement in the level of delivery to tumors (p < 0.05). The technologies and strategies described here may contribute to clinical improvements in the selectivity and efficacy of liposomal drug delivery agents.

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Sigma-Aldrich
胆固醇, Sigma Grade, ≥99%
Sigma-Aldrich
山羊抗兔IgG抗体,HRP偶联物, 1 mg/mL, Upstate®
Sigma-Aldrich
重组蛋白G, from Escherichia coli, ≥90%