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Authors Bi Y, Lee RJ, Wang X, Sun Y, Wang M, Li L, Li C, Xie J, Teng L
Received 7 May 2018
Accepted for publication 8 July 2018
Published 4 October 2018 Volume 2018:13 Pages 5811—5822
DOI https://doi.org/10.2147/IJN.S173279
Checked for plagiarism Yes
Review by Single-blind
Peer reviewers approved by Dr Govarthanan Muthusamy
Peer reviewer comments 2
Editor who approved publication: Dr Linlin Sun
Purpose: A liposome-based siRNA–drug combination was evaluated as a
potential therapeutic strategy to improve the curative effect.
Methods: A topoisomerase inhibitor SN38 prodrug was combined with a
survivin siRNA through codelivery using transferrin (Tf)-L-SN38/P/siRNA. In
this combination, SN38 was conjugated to the cell penetrating peptide TAT
through a polyethylene glycol (PEG) linker to synthesize TAT-PEG-SN38. The
amphiphilic TAT-PEG-SN38 was used as an ingredient of liposomes to improve the
cellular uptake. Protamine was added to form an electrostatic complex with
siRNA in the core of the liposomes. Tf was introduced to enable tumor cell
targeting of liposomes (Tf-L-SN38/P/siRNA).
Results: Tf-L-SN38/P/siRNA exhibited a particle size of 148 nm and a
ζ-potential of +7.8 mV. The cellular uptake and antitumor activity were
dependent on Tf receptor targeting, TAT-PEG-SN38, and siRNA codelivery.
Tf-L-SN38/P/siRNA was shown to be considerably more effective than liposomes
carrying individual components. This combination induced potent tumor
inhibition (76.8%) in HeLa cell xenograft tumor-bearing nude mice.
Conclusion: These data indicated that Tf-L-SN38/P/siRNA was an effective
system for codelivery of SN38 and a survivin siRNA and that its therapeutic
potential deserved further evaluation.
Keywords: SN38, survivin, siRNA, transferrin, prodrug