RESUMO
Various solubility-switchable ionic liquids were prepared. Their syntheses were readily achieved in a few steps from glyceraldehyde dimethylacetal or its derivatives. Pyridinium, imidazolium, and phosphonium derivatives also exhibited solubility-switchable properties; acetal-type ionic liquids were soluble in organic solvents, while diol-type ones exhibited a preference for being dissolved in the aqueous phase. The solubility of the ionic liquids prepared in this study also depended on the number of carbon atoms in the cationic parts of the ionic liquids. Interconversion between the diol-type and the acetal-type ionic liquids was readily achieved under the standard conditions for diol acetalization and acetal hydrolysis. One of the prepared ionic liquids was also examined as a solvent for an organic reaction.
RESUMO
Herein, we report the physicochemical and structural properties of a new solubility-switchable ionic liquid (IL) comprising the glycerammonium (GA) cation with a hydrophilic group, the GA cation attached to an acetal-based protective group [protected GA (PGA)], and bis(trifluoromethanesulfonyl)amide (TFSA). The interionic volumes (Vinter) of the hydrophobic [PGA][TFSA] and hydrophilic [GA][TFSA] ILs were evaluated based on solution density, revealing weaker ion-ion interactions in these relative to conventional ILs. The [PGA][TFSA] and [GA][TFSA] also exhibit poor ion-conducting properties, with up to an order of magnitude lower ionic conductivity (σ) and self-diffusion coefficient (D), as compared with conventional ILs. Radial distribution functions derived from high-energy X-ray total scattering experiments [Gexp(r)] and molecular dynamics (MD) simulations [GMD(r)] indicate that nearest-neighbor ion-ion interactions in the [PGA][TFSA] and [GA][TFSA] are comparable to those in imidazolium-based IL. Conversely, these are appreciably weakened at the second- and third-neighbors and thus less structured in the long range (r > 12 Å) and very different from the highly ordered imidazolium IL. The atom-atom pair correlation function derived from the MD simulations disclose that at a local scale, specific interactions are absent, with only an electrostatic interaction in the [PGA][TFSA], whereas the GA cations interact with TFSA anions via hydrogen bonding of diol groups in the GA and O atoms in the TFSA. No hydrogen bonding group within the PGA cation leads to weak ion-hydration resulting in a phase separation of [PGA][TFSA] and water; in contrast, the GA cations are easily hydrogen-bonded with water molecules to be miscible in aqueous solutions.
RESUMO
Chondroitin sulfate E (CS-E) plays a crucial role in diverse processes ranging from viral infection to neuroregeneration. Its regiospecific sulfation pattern, generated by N-acetylgalactosamine 4-sulfate 6-O-sulfotransferase (GalNAc4S-6ST), is the main structural determinant of its biological activity. Inhibitors of GalNAc4S-6ST can serve as powerful tools for understanding physiological functions of CS-E and its potential therapeutic leads for human diseases. A family of new 4-acylamino-ß-GalNAc derivatives and 4-azido-ß-GalNAc derivatives were synthesized for their potential application as inhibitors of GalNAc4S-6ST. The target compounds were evaluated for their inhibitory activities against GalNAc4S-6ST. The results revealed that 4-pivaloylamino- and 4-azido-ß-GalNAc derivatives displayed evident activities against GalNAc4S-6ST with IC50 value ranging from 0.800 to 0.828 mM. They showed higher activities than benzyl D-GalNAc4S that was used as control.
