Calix[4]pyrrole
phosphonate-cavitands were used as receptors for
the design of supramolecular sensors for creatinine and its lipophilic
derivative hexylcreatinine. The sensing principle is based on indicator
displacement assays of an inherently fluorescent guest dye or a black-hole
quencher from the receptor’s cavity by means of competition
with the creatinine analytes. The systems were thermodynamically and
kinetically characterized regarding their 1:1 binding properties by
means of nuclear magnetic resonance spectroscopy (1H and 31P NMR), isothermal titration calorimetry, and optical spectroscopies
(UV/vis absorption and fluorescence). For the use of the black-hole
indicator dye, the calix[4]pyrrole was modified with a dansyl chromophore
as a signaling unit that engages in Förster resonance energy
transfer with the indicator dye. The 1:1 binding constants of the
indicator dyes are in the range of 107 M–1, while hexylcreatinine showed values around (2–4) ×
105 M–1. The competitive displacement
of the indicators by hexylcreatinine produced supramolecular fluorescence
turn-on sensors that work at micromolar analyte concentrations that
are compatible with those observed for healthy as well as sick patients.
The limit of detection for one of the systems reached submicromolar
ranges (110 nM).
A general approach toward the light-induced guest release from cucurbit[7]uril by means of a photoactivatable competitor was devised. An o-nitrobenzyl-caged competitor is photolyzed to generate a competitive guest that can displace cargo from the host macrocycle solely based on considerations of chemical equilibrium. With this method the release of terpene guests from inclusion complexes with cucurbit[7]uril was demonstrated. The binding of the herein investigated terpenes, all being lead fragrant components in essential oils, has been characterized for the first time. They feature binding constants of up to 10 L mol and a high differential binding selectivity (spanning four orders of magnitude for the binding constants for the particular set of terpenes). By fine-tuning the photoactivatable competitor guest, selective and also sequential release of the terpenes was achieved.
Semisolid formulations, such as gels, creams and ointments, have recently contributed to the progression of photodynamic therapy (PDT) and microbial photodynamic inactivation (PDI) in clinical applications. The most important challenges facing this field are the physicochemical properties of photosensitizers (PSs), optimal drug release profiles, and the photosensitivity of surrounding tissues. By further integration of nanotechnology with semisolid formulations, very promising pharmaceuticals have been generated against several dermatological diseases (PDT) and (antibiotic-resistant) pathogenic microorganisms (PDI). This review focuses on the different PSs and their associated semisolid formulations currently found in both the market and clinical trials that are used in PDT/PDI. Special emphasis is placed on the advantages that the semisolid formulations bring to drug delivery in PDI. Lastly, some potential considerations for improvement in this field are also discussed.
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