Homochiral [2.2]Paracyclophane Self‐Assembly Promoted by Transannular Hydrogen Bonding

[2.2]paracyclophane (pCp), unlike many π‐building blocks, has been virtually unexplored in supramolecular constructs. Reported here is the synthesis and characterization of the first pCp derivatives capable of programmed self‐assembly into extended cofacial π‐stacks in solution and the solid state. The design employs transannular (intramolecular) hydrogen bonds (H‐bonds), hitherto unstudied in pCps, between pseudo‐ortho‐positioned amides of a pCp‐4,7,12,15‐tetracarboxamide (pCpTA) to preorganize the molecules for intermolecular H‐bonding with π‐stacked neighbors. X‐ray crystallography confirms the formation of homochiral, one‐dimensional pCpTA stacks helically laced with two H‐bond strands. The chiral sense is dictated by the planar chirality (R_p or S_p) of the pCpTA monomers. A combination of NMR, IR, and UV/Vis studies confirms the formation of the first supramolecular pCp polymers in solution.     

Isolable Chiral Aggregates of Achiral π‐Conjugated Carboxylic Acids

The induced aggregation of achiral building blocks by a chiral species to form chiral aggregates with memorized chirality has been observed for a number of systems. However, chiral memory in isolated aggregates of achiral building blocks remains rare. One possible reason for this discrepancy could be that not much is understood in terms of designing these chiral aggregates. Herein, we report a strategy for creating such isolable chiral aggregates from achiral building blocks that retain chiral memory after the facile physical removal of the chiral templates. This strategy was used for the isolation of chiral homoaggregates of neutral achiral π‐conjugated carboxylic acids in pure aqueous solution. Under what we have termed an “interaction–substitution” mechanism, we generated chiral homoaggregates of a variety of π‐conjugated carboxylic acids by using carboxymethyl cellulose (CMC) as a mediator in acidic aqueous solutions. These aggregates were subsequently isolated from the CMC templates whilst retaining their memorized supramolecular chirality. Circular dichroism (CD) spectra of the aggregates formed in the acidic CMC solution exhibited bisignated exciton‐coupled signals of various signs and intensities that were maintained in the isolated pure homoaggregates of the achiral π‐conjugated carboxylic acids. The memory of the supramolecular chirality in the isolated aggregates was ascribed to the substitution of COOH/COOH hydrogen‐bonding interaction between the carboxylic acid groups within the aggregates for the hydrogen‐bonding interactions between the COOH groups of the building blocks and the chiral templates. We expect that this “interaction–substitution” procedure will open up a new route to isolable pure chiral aggregates from achiral species.     

Topological classification and supramolecular chirality of 21-helical ladder-type hydrogen-bond networks composed of primary ammonium carboxylates: bundle control in 21-helical assemblies

The supramolecular chirality of 1D ladder-type hydrogen-bond networks composed of primary ammonium carboxylates was determined based on topological considerations. Chirality in such networks is based on the absolute configuration of the primary ammonium cation, which arises from discrimination between the two oxygen atoms of the carboxylate anion. The configurations of the cations and anions generate topological diversity in the networks, which are classified into six subgroups. In the Cambridge Structural Database, salts based on ladder type 1 constitute over 70 % of salts with a 1D-ladder-type network. Ladder type 1, based on a 2(1)-axis, is not superimposable on its mirror image, which leads to the first definition of right- or left-handedness of 2(1)-helicity on the basis of supramolecular tilt chirality. Helical assemblies of 2(1)-type with triaxial chirality can be assembled in various ways to yield chiral bundles and crystals. On the basis of these considerations, we constructed clay mimic structures with several bundle patterns by connecting the hydrogen-bond networks by using bifunctional molecules. These results open up the possibility of in-depth crystal engineering based on hydrogen-bond topology.     

三维超分子[Ni(hmt)2(SCN)2(H2O)2][Ni(SCN)2(H2O)4](H2O)2的自组装,晶体结构及磁性质(hmt=六次甲基四胺)

Compound [Ni(hmt)₂(SCN)₂(H₂O)₂][Ni(SCN)₂(H₂O)₄](H₂O)₂ (hmt=hexamethylenetetramine) was pre-pared and structurally characterized by means of X-ray single crystal diffraction. The two neutral units [Ni(hmt)₂(SCN)₂(H₂O)₂] and [Ni(SCN)₂(H₂O)₄] are joined together through hydrogen bonds N…H-O, O…H-O and S…H-O. In the solid state, the compound has three-dimensional network structure. The determination of its variable-temperature magnetic susceptibilities (5～300K) shows that the magnetic behavior obeys the Curie-Weiss law over the whole temperature ranges.     

Autoamplification of Molecular Chirality through the Induction of Supramolecular Chirality

The novel concept for the autoamplification of molecular chirality, wherein the amplification proceeds through the induction of supramolecular chirality, is presented. A solution of prochiral, ring‐open diarylethenes is doped with a small amount of their chiral, ring‐closed counterpart. The molecules co‐assemble into helical fibers through hydrogen bonding and the handedness of the fibers is biased by the chiral, ring‐closed diarylethene. Photochemical ring closure of the open diarylethene yields the ring‐closed product, which is enriched in the template enantiomer.     

Amplification of chirality in dynamic supramolecular aggregates

The quest to understand the origin of chirality in biological systems has evoked an intense search for nonlinear effects in catalysis and pathways to amplify slight enantiomeric excesses in racemates to give optically pure molecules. The amplification of chirality in polymeric systems as a result of cooperative processes has been intensely investigated. Ten years ago, this effect was shown for the first time in noncovalent dynamic supramolecular systems. Since then, it has become clear that a subtle interplay of noncovalent interactions such as hydrogen-bonding, pi-pi stacking, and hydrophobic interactions is also sufficient to observe amplification of chirality in small molecules. Here we summarize the results obtained over the past decade and the general guidelines we can deduce from them. Predicting amplification of chirality is still impossible, but it appears to be a balance between different types of interactions, the formation of an intrinsically chiral object, and cooperative aggregation processes.     

Multivalent C−H⋅⋅⋅Cl/Br−C Interactions Directing the Resolution of Dynamic and Twisted Capsules

In this work, we report a mechanism by which stereoisomeric and twisted capsules P/M- 1 direct their dynamic chirality in the presence of haloalkane guests. The capsule comprises a static, but twisted, cage that is linked to a dynamic tris(2-pyridylmethyl)amine (TPA) lid at its top. From the results of experimental (NMR spectroscopy and X-ray crystallography) and computational (DFT) studies, the TPA lid was shown to assume clockwise (+) and counterclockwise (−) folds with diastereomeric (but racemic) capsules M- 1 (+) and M- 1 (−) interconverting at a rapid rate (ΔG^≠_189K=9.1 kcal mol⁻¹). The relative stability of the capsules was found to be a function of guest(s) residing in their interior (243/262 ų) with small CH₂Cl₂ (61 ų) yielding roughly equal population of diastereomeric inclusion complexes. Larger guests, such as CCl₄ (89 ų) and CBr₄ (108 ų), however, formed M- 1 (−)⊂CX₄ at the expense of M- 1 (+)⊂CX₄ in circa 3:1 ratio. To account for the observation, theory (DFT:M06-2X/6–31+G*) and experiments (¹H NMR spectroscopy) were used to deduce that CX₄ guests become localized inside the twisted cage of the capsule by forming a C−X⋅⋅⋅π halogen bond [N_c=d/(r_H+r_X)=0.91–0.92] with the benzene “floor” while encountering electrostatic repulsions with closer naphthalimide boundaries. At last, the TPA lid used its central methylene hydrogens to establish, within the M- 1 (−)⊂CX₄, three stabilizing C−H⋅⋅⋅X−C interactions with the guest. The same C−H⋅⋅⋅X−C interactions, however, became weaker (or possibly vanished) after the conformational reorganization of the lid and the formation of less stable M- 1 (+)⊂CX₄ complex. On individual basis, C−H⋅⋅⋅X−C intermolecular contacts are weak and hardly detectable in the solution phase. In the case of capsule P/M- 1 , however, these contacts were multivalent and altogether strong enough to direct the host's dynamic chirality.     

Self-assembly of folic acid derivatives: induction of supramolecular chirality by hierarchical chiral structures

Hierarchical chiral structures made up of dendritic oligo(L- or D-glutamic acid) moieties of folic acid derivatives induce supramolecular chirality in the self-assembled columnar structures of the folic acids. These folic acids self-assemble through the intermolecular hydrogen bonds of the pterin rings to form disklike tetramers. In the neat states, the stacked tetramers form thermotropic hexagonal columnar phases over wide temperature ranges, including room temperature. Addition of alkali metal salts induces chirality in the columnar phases. In dilute solution states in a relatively polar solvent (chloroform), the folic acid derivatives form non-chiral, self-assembled structures. In the presence of sodium triflate, the folic acid forms chiral columnar assemblies through the oligo(L-glutamic acid) moiety, similar to those formed in the liquid-crystalline (LC) states. The enantiomer of the folic acid induces columnar assemblies with reversed helicity. In the case of the diastereomer, no induced helicity is observed. Application of an apolar solvent (dodecane) drives the folic acid derivatives to form chiral assemblies in the absence of ions. In this case, lipophilic interactions promote nanophase segregation, which enhances the formation of chiral columns. Interestingly, the chiral supramolecular structure of the diastereomer induces the most intense circular dichroism. In both cases, the molecular chirality in the oligo(glutamate) moieties yields supramolecular chirality of the folic acids that self-assemble through cooperative molecular interactions.