Affiliation:
1. Department of Chemistry, University of Ioannina, Ioannina 45110, Greece
2. Department of Chemistry, National and Kapodistrian University of Athens, Panepistimiopolis Zografou 15771, Greece
Abstract
Drugs have to overcome numerous barriers to reach their desired therapeutic targets.
In several cases, drugs, especially the highly lipophilic molecules, suffer from low solubility
and bioavailability and therefore their desired targeting is hampered. In addition, undesired
metabolic products might be produced or off-targets could be recognized. Along these
lines, nanopharmacology has provided new technological platforms, to overcome these
boundaries. Specifically, numerous vehicle platforms such as cyclodextrins and calixarenes
have been widely utilized to host lipophilic drugs such as antagonists of the angiotensin II
AT1 receptor (AT1R), as well as quercetin and silibinin. The encapsulation of these drugs in
supramolecules or other systems refines their solubility and metabolic stability, increases their
selectivity and therefore decreases their effective dose and improves their therapeutic index.
In this mini review we report on the formulations of silibinin and AT1R antagonist candesartan
in a 2-HP-β-cyclodextrin host molecule, which displayed enhanced cytotoxicity and increased
silibinin’s and candesartan’s stability, respectively. Moreover, we describe the encapsulation
of quercetin in gold nanoparticles bearing a calixarene supramolecular host. Also, the
encapsulation of temozolomide in a calixarene nanocapsule has been described. Finally, we
report on the activity enhancement that has been achieved upon using these formulations as
well as the analytical and computational methods we used to characterize these formulations
and explore the molecular interactions between the host and quest molecules.
Publisher
Bentham Science Publishers Ltd.
Subject
Pharmacology,Molecular Medicine,Drug Discovery,Biochemistry,Organic Chemistry
Cited by
8 articles.
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