Owing to their characteristic structures,
metal–organic
frameworks (MOFs) are considered as the leading candidate for drug-delivery
materials. However, controlling the synthesis of MOFs with uniform
morphology and high drug-loading/release efficiencies is still challenging,
which greatly limits their applications and promotion. Herein, a multifunctional
MOF-based drug-delivery system (DDS) with a controlled pore size of
100–200 nm for both therapeutic and bioimaging purposes was
successfully synthesized in one step. Fe-MOF-based microcapsules were
synthesized through a competitive coordination method, which was profited
from the intrinsic coordination characteristics of the Fe element
and the host-guest supramolecular interactions between Fe3+ and polyoxometalates anions. This as-synthesized macroporous DDS
could greatly increase the drug-loading/release rate (77%; 83%) and
serve as a magnetic resonance (MR) contrast agent. Because an Fe-containing
macroporous DDS presents ultrahigh drug loading/release, the obtained
5-FU/Fe-MOF-based microcapsules displayed good biocompatibility, extremely
powerful inhibition of tumor growth, and satisfactory MR imaging capability.
Given all these advantages, this study integrates high therapeutic
effect and diagnostic capability via a simple and effective morphology-controlling
strategy, aiming at further facilitating the applications of MOFs
in multifunctional drug delivery.
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