Polycationic Nanofibers for Nucleic Acid Scavenging.

Dying cells release nucleic acids (NA) and NA-containing complexes that activate inflammatory pathways of immune cells. Sustained activation of these pathways contributes to chronic inflammation frequently encountered in autoimmune and inflammatory diseases. In this study, grafting of cationic polymers onto a nanofibrous mesh enabled local scavenging of negatively charged pro-inflammatory molecules in the extracellular space. Nucleic acid scavenging nanofibers (NASFs) formed from poly(styrene-alt-maleic anhydride) conjugated with 1.8 kDa bPEI resulted in nanofibers of diameters 486 ± 9 nm. NASFs inhibited the NF-κB response stimulated by the negatively charged agonists, CpG and poly(I:C), in Ramos-blue cells but not Pam3CSK4, a nonanionic agonist. Moreover, NASFs significantly impeded NF-κB activation in cells stimulated with damage-associated molecular pattern molecules (DAMPs) released from doxorubicin killed cancer cells. In vivo application of NASFs to open wounds demonstrated nucleic acid scavenging in wounds of diabetic mice infected with Pseudomonas aeruginosa, suggesting the in vivo efficacy of NASFs. This simple technique of generating NASF results in effective localized anti-inflammation in vitro and local nucleic acid scavenging in vivo.

Anion-controlled foldamers.

This tutorial review provides a summary of anion-mediated folding of linear and cyclic oligomers as well as anion-responsive behaviours of related polymeric architectures. Anions have emerged as a significant focus of the supramolecular community and here we review their impact on directing the secondary structures of synthetic oligomers and polymers while modulating physical properties e.g. molecular recognition. Oligomers and polymers responsive to anionic guests are typically constructed with hydrogen bond donors complementary to the target anions. Anion binding within the cavities leads to folding and helical wrapping of linear and cyclic oligomers as well as control over macromolecular properties of polymers. This review covers the impact of anion binding on guiding the secondary structures of single-stranded folded oligomers (foldamers) and cyclic oligomers (macrocycles), and on modulating the physical properties of select polymer architectures.

Selective sulfate binding induces helical folding of an indolocarbazole oligomer in solution and solid state.

Hydrogen bonding to anions drives the helical folding of an indolocarbazole oligomer, thus resulting in an internal cavity with six NHs and two OHs for binding sulfate with high selectivity.

Anion binding of short, flexible aryl triazole oligomers.

The flexible, electropositive cavity of linear 1,4-diaryl-1,2,3-triazole oligomers provides a suitable host for complexation of various anions. The binding affinities for various combinations of oligomer and anion were determined by (1)H NMR titrations. Effective ionic radius is found to be a primary determinant of the relative binding interactions of various guests, with small but measurable deviations in the case of nonspherical anions. Solvent effects are significant, and the strength of the binding interaction is found to depend directly on the donor ability of the solvent. A picture emerges in which anion binding can be effectively interpreted in terms of a competition between two solvation spheres: one provided by the solvent and a second dominated by a folded cavity lined with electropositive 1,2,3-triazole CH protons. Implications for rigid macrocycles and other multivalent hosts are discussed.

Foldamers with helical cavities for binding complementary guests.

This tutorial review provides a summary of the binding of neutral molecules, cations and anions within helical cavities formed specifically by the folding of unnatural oligomers, called foldamers. Foldamers are emerging as a new class of synthetic receptors whose binding sites are not formed by preorganization of covalent bonds, but rather through the combination of various noncovalent interactions that induce folding and subsequent arrangement of functional groups within a helical cavity. The function of foldamers as synthetic receptors can be tuned by careful selection of modular building blocks displaying the appropriate functionality required for guest complexation. As the molecular toolbox expands to create well-defined helical structures, new and interesting functions emerge. It is the purpose of this review to provide the reader with an introduction to helical cavities formed specifically by foldamers and their subsequent function as molecular and ionic receptors. It will interest the supramolecular, organic and bioorganic communities.

Orthogonal control of dissociation dynamics relative to thermodynamics in a main-chain reversible polymer.

A pair of homologous and soluble reversible polymers display nearly identical solution structures but dramatically different dissociation dynamics (1.0 vs ca. 100 s-1) along their main chains. The polymers are formed by organopalladium-pyridine coordination, and steric effects at the metal center control the dynamics. Importantly, the association constant is not significantly affected by the sterics. The resulting orthogonal control over dissociation kinetics provides a general tool for studying the effects of dynamics independent of thermodynamics in supramolecular systems, particularly main-chain reversible polymers.