One-Pot Synthesis of Mesoporous
Silica Nanocarriers with Tunable Particle Sizes and Pendent Carboxylic
Groups for Cisplatin Delivery
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Abstract
Mesoporous silica nanocarriers with tunable particle
sizes and different loadings of pendent carboxylic groups were successfully
prepared by a straightforward and reproducible strategy, in which
carboxyethylsilanetriol sodium salt was co-condensed with tetraethoxyorthosilicate
to introduce the carboxylic groups. The key in this strategy was to
separate the synthesis process into two steps of the nuclei formation
and particle growth. The uniform particle size and ordered structure
of the synthesized nanocarriers were manifested by several techniques
such as XRD, TEM, SEM, and BET. DLS measurement illustrated that nanocarriers
could be well suspended in aqueous solution. The integration and content
tunability of the carboxylic groups within mesoporous silica nanoparticles
(MSNs) were verified by FT-IR and <sup>29</sup>Si NMR. The inherent
carboxylic units on the obtained carboxylic group modified MSNs (MSNs-C)
effectively enhanced the capture and tailored the release properties
of the anticancer drug of cisplatin. The accumulation of drug in the
HeLa cells was greatly enhanced due to the highly efficient platinum
uptake efficiency transported by the synthesized nanocarriers. The
drug encapsulated in the MSNs-C exhibited a higher antitumor activity
than free cisplatin against both MCF-7 and HeLa cells