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Anticancer activity of the intraperitoneal-delivered DFP-10825, the cationic liposome-conjugated RNAi molecule targeting thymidylate synthase, on peritoneal disseminated ovarian cancer xenograft model
Authors Iizuka K, Jin C, Eshima K, Hong MH, Eshima K, Fukushima M
Received 9 November 2017
Accepted for publication 4 January 2018
Published 29 March 2018 Volume 2018:12 Pages 673—683
DOI https://doi.org/10.2147/DDDT.S156635
Checked for plagiarism Yes
Review by Single-blind
Peer reviewers approved by Dr Rammohan Devulapally
Peer reviewer comments 2
Editor who approved publication: Dr Georgios Panos
Introduction: Peritoneal disseminated ovarian cancer is one of the most difficult
cancers to treat with conventional anti-cancer drugs and the treatment options
are very limited, although an intraperitoneal (ip) paclitaxel has shown some
clinical benefit. Therefore, treatment of peritoneal disseminated ovarian
cancer is a highly unmet medical need and it is urgent to develop a new ip
delivered drug regulating the fast DNA synthesis.
Methods: We
developed a unique RNAi molecule consisting of shRNA against the thymidylate
synthase (TS) and a cationic liposome (DFP-10825) and tested its antitumor
activity and PK profile in peritoneally disseminated human ovarian cancer
ascites models by the luciferase gene-transfected SCID mice. DFP-10825 alone,
paclitaxel alone or combination with DFP-10825 and paclitaxel were administered
in an ip route to the tumor-bearing mice. The TS expression level was measured
by conventional RT-PCR. The anti-tumor activity and host survival benefit by
DFP-10825 treatment on tumor-bearing mice were observed as resulting from the
specific TS mRNA knock-down in tumors.
Results: DFP-10825 alone significantly suppressed the growth of
SKOV3-luc tumore ascites cells and further extended the survival time of these
tumor-bearing mice. Combination with the ip paclitaxel augmented the antitumor
efficacy of DFP-10825 and significantly prolonged the survival time in the
tumor-bearing mice. Short-hairpin RNA for TS (TS shRNA) levels derived from
DFP-10825 in the ascetic fluid were maintained at a nM range across
24 hours but not detected in the plasma, suggesting that TS shRNA is
relatively stable in the peritoneal cavity, to be able to exert its anti-tumor
activity, but not in blood stream, indicating little or no systemic effect.
Conclusion: Collectively, the ip delivery of DFP-10825, TS shRNA
conjugated with cationic liposome, shows a favorable antitumor activity without
systemic adverse events via the stable localization of TS shRNA for a
sufficient time and concentration in the peritoneal cavity of the peritoneally
disseminated human ovarian cancer-bearing mice.
Keywords: DFP-10825,
thymidylate synthase, short-hairpin RNA, cationic liposome, ip delivery,
intraperitoneal dissemination, ovarian cancer
摘要视频链接:IP chemotherapy with
DFP-10825, TSshRNA-liposome
