Transferrin conjugation does not increase the efficiency of liposomal Foscan during in vitro photodynamic therapy of oesophageal cancer
File Type:
PDFItem Type:
Journal ArticleDate:
2013Access:
OpenAccessCitation:
E Paszko, GM Vaz, C Ehrhardt, MO Senge, Transferrin conjugation does not increase the efficiency of liposomal Foscan during in vitro photodynamic therapy of oesophageal cancer, European Journal of Pharmaceutical Sciences, 48, 1-2, 2013, 202-210Download Item:
Abstract:
Photodynamic therapy (PDT) is based on the delivery of photocytotoxic agents to a target
tissue, followed by irradiation. In order to increase the efficiency of PDT in oesophageal
cancer therapy, polyethylene glycol (PEG)-grafted, transferrin (Tf)-conjugated liposome
formulations of 5,10,15,20-tetra(m-hydroxyphenyl)chlorin (Foscan), a second-generation
photosensitiser, were prepared. Expression of transferrin receptors (CD71) in the oesophageal
cancer cell line, OE21, was confirmed by immunoblot and confocal laser scanning
microscopy. The anti-proliferative effect of Foscan liposomes was evaluated and compared
with plain formulations (i.e., without Tf) as well as with free drug. In addition, the
intracellular accumulation was studied using high content analysis. Surprisingly, delivering
Foscan by transferrin-conjugated PEG-liposomes to oesophageal cancer cells did not improve
the photocytotoxicity or the intracellular accumulation of Foscan when compared to
unmodified liposomes or indeed free photosensitiser. Tf-targeted drugs and drug delivery
systems have shown improvedthe therapy of many cancers. Our study, however, did not
corroborate these findings. If this is due to the tumour type, the choice of in vitro model or
the delivery systems remains to be confirmed.
Sponsor
Grant Number
Health Research Board (HRB)
Author's Homepage:
http://people.tcd.ie/ehrhardchttp://people.tcd.ie/sengem
Description:
PUBLISHEDType of material:
Journal ArticleCollections
Series/Report no:
European Journal of Pharmaceutical Sciences48
1-2
Availability:
Full text availableSubject (TCD):
CancerDOI:
http://dx.doi.org/10.1016/j.ejps.2012.10.018Metadata
Show full item recordLicences: