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负载柔红霉素的 PLGA-PLL-PEG-Tf 纳米粒子在血液系统恶性肿瘤中的应用:体外和体内评估
Authors Bao W, Liu R, Xia G, Wang F, Chen B
Received 26 November 2018
Accepted for publication 19 February 2019
Published 8 April 2019 Volume 2019:13 Pages 1107—1115
DOI https://doi.org/10.2147/DDDT.S195832
Checked for plagiarism Yes
Review by Single-blind
Peer reviewers approved by Dr Andrew Yee
Peer reviewer comments 2
Editor who approved publication: Dr Anastasios Lymperopoulos
Background: With the
development of drug delivery, novel tools and technological approaches have
captured the attention of researchers in recent years. Several target drug
delivery systems (DDSs) including nanoparticles (NPs) have been developed as an
important strategy to deliver classical medicine.
Objective: The
objective of this study was to evaluate the application of novel daunorubicin
(DNR)-loaded poly(lactic-co-glycolic acid)-poly-l-lysine-polyethylene
glycol-transferrin (Tf) nanoparticles (DNR-loaded NPs) in hematologic
malignancies in vitro and in vivo.
Materials and methods: DNR-loaded
NPs were prepared by the modified double-emulsion solvent evaporation/diffusion
method, and its microscopic form was observed under scanning electron
microscope. Intracellular distribution of DNR was directly detected by
fluorescence microscopy. After establishment of a tumor xenograft model by
injecting K562 cells into the left leg of nude mice, the therapeutic effect of
the DNR-loaded NPs on the growth of tumors was measured by calculating the
tumor size, and the relative expression of Caspase-3 protein was detected by
immunohistochemical staining. Furthermore, intracellular concentration of DNR
and the extent of cell apoptosis in primary leukemia cells were quantified by
flow cytometry.
Results: DNR-loaded
NPs had a spherical shape of about 180 nm in diameter. DNR-loaded NP group
showed a significant enhancement of cellular uptake in K562 cells compared with
DNR group. Tumor inhibition rate was higher in DNR-loaded NP group in
comparison with DNR group, and the relative expression of Caspase-3 protein was
upregulated in DNR-loaded NP group compared with DNR group. Furthermore,
DNR-loaded NPs obviously increased intracellular concentration of DNR in
primary leukemia cells compared with DNR group, but there was no significant
difference in primary cell apoptosis between the two groups. These findings
suggest that the novel NP DDS can enhance the performance of conventional
antitumor drugs and may be suitable for further application in the treatment of
hematologic malignancies.
Keywords: nanoparticles,
transferrin, targeted drug delivery system, leukemia
