ABSTRACT
A new calixpyridinium-based light-responsive host-guest recognition motif was found in this work. This host-guest recognition motif was further discovered to be applied as a selective turn-on fluorescent sensor for lysine over other natural amino acids.
Subject(s)
Fluorescent Dyes/chemistry , Lysine/chemistry , Macrocyclic Compounds/chemistry , Photolysis , Pyridinium Compounds/chemistry , Biosensing Techniques/methods , Hydrophobic and Hydrophilic Interactions , Molecular Conformation , Spectrometry, Fluorescence , WaterABSTRACT
In this work, cationic macrocyclic calixpyridinium was employed as a new strategy to condense DNA. Moreover, the degradation of DNA by DNase I could lead to the calixpyridinium-DNA supramolecular aggregates being dissipated. Therefore, the present system is potentially applicable as the targeted drug delivery model at DNase I-overexpressed sites.
Subject(s)
Calixarenes/chemistry , DNA/chemistry , Deoxyribonuclease I/chemistry , Animals , SalmonABSTRACT
The information in the literature concerned with lowering the critical aggregation concentration of anionic surfactants by macrocyclic compounds is scarce. This research develops an effective route for lowering the critical aggregation concentration of anionic gemini surfactants by the complexation of calixpyridinium. Furthermore, the size of complex self-assembled nanostructures can be well controlled by the different mixing ratio of the host and the guest.
Subject(s)
Pyridinium Compounds/chemistry , Surface-Active Agents/chemical synthesis , Nanoparticles/chemistry , Surface-Active Agents/chemistryABSTRACT
In this work, a comparative study on the supramolecular assemblies formed by calixpyridinium and two alginates with different viscosities was performed. We found that sodium alginate (SA) with medium viscosity (SA-M) had a better capability to induce aggregation of calixpyridinium in comparison with SA with low viscosity (SA-L) because of the stronger electrostatic interactions between calixpyridinium and SA-M. Therefore, the morphology of calixpyridinium-SA-M supramolecular aggregates was a compact spherical structure, while that of calixpyridinium-SA-L supramolecular aggregates was an incompact lamellar structure. As a result, adding much more amount of 1,3,6,8-pyrenetetrasulfonic acid tetrasodium salt to calixpyridinium-SA-M solution was required to achieve the balance of the competitive binding, and in comparison with calixpyridinium-SA-L supramolecular aggregates, calixpyridinium-SA-M supramolecular aggregates were more sensitive to alkali. However, for the same reason, in comparison with calixpyridinium-SA-M supramolecular aggregates, calixpyridinium-SA-L supramolecular aggregates were much more stable in water not only at room temperature but also at a higher temperature, and even in salt solution. Therefore, in comparison with calixpyridinium-SA-L supramolecular aggregates, calixpyridinium-SA-M supramolecular aggregates exhibited a completely opposite response to acid because of the generation of salt. Because SA is an important biomaterial with excellent biocompatibility, it is anticipated that this comparative study is extremely important in constructing functional supramolecular biomaterials.
ABSTRACT
We have successfully constructed a supramolecular assembly based on the anionic recognition of calixpyridinium for the first time employing native biocompatible polysaccharide hyaluronan as the guest, which showed hyaluronidase-responsive disassembly and temperature-responsive morphological conversion from a nanosphere to a nanosquare upon increasing the temperature.
ABSTRACT
The molecular binding behavior of water-soluble calix[4]arenes (p-sulfonatocalix[4]arene (SC4A) and p-sulfonatothiacalix[4]arene (STC4A)) with two asymmetric 4,4'-bipyridinium guests (N-methyl-N'-adamantane carbomethyl-4,4'-bipyridinium dibromide (MVAd2+) and N-methyl-N'-(naphthalen-2-ylmethyl)-4,4'-bipyridinium bromide iodide (MVNp2+)) was systematically studied using NMR spectroscopy and microcalorimetry in a neutral aqueous solution. Either the methyl group or the adamantane moiety in MVAd2+ could enter into the SC4A and STC4A cavities, without regioselectivity. The STC4A cavity can also accommodate MVNp2+, either through incorporation of the methyl group or the naphthalene moiety, without regioselectivity. However, we were surprised to find that MVNp2+ could only be included within the SC4A cavity through incorporation of the methyl group, with regioselectivity, which is rare for a flexible host. Furthermore, both SC4A and STC4A can form stable inclusion complexes with the two investigated asymmetric 4,4'-bipyridinium guests, driven by very favorable enthalpy changes, and the thermodynamic origins of the host selectivities for MVAd2+ and MVNp2+ can be well explained through their binding modes. The finding of this novel regioselective recognition is promising for potential applications in the development of more sophisticated biomimetic materials.
ABSTRACT
We have successfully implemented the supramolecular tandem assay principle for the real-time, continuous, direct, and label-free monitoring of alkaline phosphatase activity through a fluorescence "switch-off" assay based on a novel calixpyridinium/dye reporter pair. Because several diseases can be preliminarily diagnosed in light of an abnormal level of alkaline phosphatase in serum, the application of tandem assays to selectively monitor alkaline phosphatase activity has feasible implications in disease diagnosis.
Subject(s)
Adenosine Triphosphate/metabolism , Alkaline Phosphatase/metabolism , Enzyme Assays/methods , Pyridines/metabolism , Alkaline Phosphatase/analysis , Fluorescent Dyes/chemistry , Fluorescent Dyes/metabolism , Hydrolysis , Macromolecular Substances/chemistry , Macromolecular Substances/metabolism , Molecular Structure , Pyridines/chemistryABSTRACT
The binding modes, inclusion abilities, and thermodynamic parameters for the intermolecular complexation of p-sulfonatocalix[4]arene (SC4A), p-sulfonatocalix[5]arene (SC5A), and p-sulfonatothiacalix[4]arene (STC4A), with methyl viologen (MV(2+)), ethyl viologen (EV(2+)), propyl viologen (PV(2+)), butyl viologen (BV(2+)), and benzyl viologen (BnV(2+)), were systematically investigated by NMR spectroscopy, molecular mechanics calculation, and microcalorimetry in neutral aqueous solutions. The obtained results show that all the sulfonated calixarene hosts can form stable inclusion complexes with viologen guests driven by much favorable enthalpy changes. All the viologen guests are encapsulated into the smaller SC4A cavity in their axial orientation. The larger SC5A cavity can accommodate all the viologen guests at its upper-rim midsection in the latitudinal orientation. The binding modes of more flexible STC4A with the smaller MV(2+) and EV(2+) guests are similar to those of SC5A with the two guests, while the binding modes of STC4A with the larger PV(2+) and BV(2+) guests are similar to those of SC4A with the two guests. The host selectivity for all the investigated viologen guests is the same: SC5A > SC4A > STC4A. The magnitude of the host selectivity is associated with the size of the guest. Moreover, the thermodynamic origin of the host selectivity for these viologen guests can be explained well by host-guest binding modes.
