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Effect of delivery system on the pharmacokinetic and phototherapeutic properties of bis(methyloxyethyleneoxy)silicon-phthalocyanine in tumor-bearing mice
Authors:D. W  hrle, S. Muller, M. Shopova, V. Mantareva, G. Spassova, F. Vietri, F. Ricchelli,G. Jori
Affiliation:

aInstitute of Organic and Macromolecular Chemistry, University of Bremen, PO Box 33 04 40, D-28334 Bremen, Germany

bInstitute of Organic Chemistry, Bulgarian Academy of Sciences, 1113 Sofia, Bulgaria

cClinica Chirurgica, Università di Roma, Rome, Italy

dCNR Centre of Metalloproteins and Department of Biology, University of Padua, I-35121 Padua, Italy

Abstract:A Si(IV)-phthalocyanine bearing two methoxyethyleneglycol axial ligands bound to the central metal ion (SiPc) has been prepared by chemical synthesis and analyzed for its phototherapeutic activity after administration in a Cremophor or liposome formulation to C57B1/6 mice bearing a subcutaneously transplanted Lewis lung carcinoma (LLC). The maximum drug accumulation in the tumor is found at 24 h after intraperitoneal injection, independent of the delivery system. However, the tumor concentration of SiPc in the Cremophor formulation is about two-fold higher, while the drug concentration in liver and skin shows similar trends with the two delivery systems. The drug accumulation and retention in the brain is much larger when using Cremophor emulsion. Photodynamic therapy (672 nm, 370 mW m−2, 360 J cm−2) at 24 h after the injection of Cremophor emulsion- or DPPC liposome-formulated SiPc causes a very efficient and similar response for the LLC (8 versus 22 mm mean tumor diameter for the control groups at 21 days after phototreatment). These very promising effects, obtained both at higher and lower tumor drug concentrations, clearly demonstrate the potential phototherapeutical activity of the newly synthesized SiPc.
Keywords:Axial ligands   Cremophor EL   Liposomes   Pharmacokinetics   Photodynamic therapy   Si(IV)-phthalocyanine   Tumor model
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