4.6 Article

Stimuli-Responsive Amphiphilic Pillar[n]arene Nanovesicles for Targeted Delivery of Cancer Drugs

Journal

ACS OMEGA
Volume 6, Issue 40, Pages 25876-25883

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsomega.1c04297

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Funding

  1. American University in Cairo

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Supramolecular nanovesicles, including pillar[n]arenes, have emerged as potential smart nanocarriers for cancer chemotherapeutics, offering high encapsulation capacity and controlled drug release capabilities. Their use in cancer targeted drug delivery has shown promise due to their symmetric structure, ease of functionalization, and biocompatibility.
Cancer chemotherapeutics face several challenges, including uncontrollable drug release, off-target toxic effects, and poor bioavailability. Recently, supramolecular nanovesicles, such as calix[n]arenes (CXs), cyclodextrins (CDs), cucurbiturils (CBs), and pillar[n]arenes (PRs), have attracted attention as potential smart nanocarriers for chemotherapeutics because of their exceptional cavities that can achieve high encapsulation capacity and accommodate both hydrophilic and hydrophobic drugs. In addition, they can be functionalized with different stimuli-responsive groups, which facilitate controlled drug release. Supramolecular nanovesicles, loaded with drugs and decorated with stimuli-responsive targeting moieties, are designed by either host-guest complexation or self-assembly of amphiphilic cavitands. Pillar[n]arenes, in particular, are novel supramolecular host molecules that have recently been employed in cancer targeted drug delivery because of their symmetric pillar-shaped structure, simplicity of functionalization, and biocompatibility. This review summarizes state-of-the-art strategies for developing single or multiple stimuli-responsive pillar[n]arene nanovesicles for effective cancer treatment.

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