Silk
fibroin (SF) is a biomacromolecule that can be assembled into
nanostructures and induce biomimetic nucleation of inorganic materials.
Zeolitic imidazolate framework-8 (ZIF-8), a metal–organic framework
(MOF), can be dissolved selectively under acidic pH. Here, we integrated
SF and ZIF-8 to develop novel drug carriers that selectively release
drug in the acidic intracellular environment of cancer cells. Specifically,
SF was assembled into nanoparticles (SF-NPs), which were then loaded
with an antitumor drug, doxorubicin (DOX), to form DSF-NPs. Due to
the SF-mediated organization of ZIF-8 precursors such as zinc ions,
the DSF-NPs further templated the nucleation of ZIF-8 onto their surface
to generate core–shell-structured NPs (termed DSF@Z-NPs) with
ZIF-8 as a shell and DSF-NP as a core. We found that the DSF@Z-NPs,
highly stable under neutral conditions, could be uptaken by breast
cancer cells, release DOX selectively owing to dissolution of ZIF-8
shells in the acidic intracellular environment in a controlled manner,
and induce cell apoptosis. We also confirmed that the DSF@Z-NPs could
inhibit tumor growth more efficiently to reach a higher survival rate
than their controls by inducing cell apoptosis in vivo. Our study
suggests that SF and MOF could be combined to design a new type of
cancer therapeutics.
Highly optically pure homochiral 1-(4-alkylthiophenyl) alcohols were prepared efficiently and practically via the oxazaborolidine-catalyzed asymmetric borane reduction of prochiral ketones in toluene at 25 degrees C. The coordination of the sulfur atom in the ketones to the boron atom in the catalyst and borane can be inhibited under these reduction conditions.
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