Supramolecular Photochirogenesis with a Higher-Order Complex: Highly Accelerated Exclusively Head-to-Head Photocyclodimerization of 2-Anthracenecarboxylic Acid via 2:2 Complexation with Prolinol.

An unprecedented 2:2 complex was shown to intervene in the enantiodifferentiating photocyclodimerization of 2-anthracenecarboxylic acid (A) mediated by a hydrogen-bonding template l-prolinol (P) to accelerate the formation of chiral anti-head-to-head and achiral syn-head-to-head cyclodimers in >99% combined yield with enhanced enantioselectivities of up to 72% ee for the former. The supramolecular complexation and photochirogenic behaviors, as well as the plausible structures, of intervening Am·Pn complexes (m, n = 1 or 2) were elucidated by combined theoretical and experimental spectroscopic, photophysical, and photochemical studies. Furthermore, the photochemical chiral amplification was achieved for the first time by utilizing the preferential 2:2 complexation of A with homochiral P to give normalized product enantioselectivities higher than those of the template used. The present strategy based on the higher-order hydrogen-bonding motif, which is potentially applicable to a variety of carboxylic acids and ß-aminoalcohols, is not only conceptually new and expandable to other (photo)chirogenic and sensing systems but also may serve as a versatile tool for achieving photochemical asymmetric amplification and constructing chiral functional supramolecular architectures.

Synthesis and radical-scavenging activity of a dimethyl catechin analogue.

Catechin analogue 1 with methyl substituents ortho to the catechol hydroxyl groups was synthesized to improve the antioxidant ability of (+)-catechin. The synthetic scheme involved a solid acid catalyzed Friedel-Crafts coupling of a cinnamyl alcohol derivative to 3,5-dibenzyloxyphenol followed by hydroxylation and then cyclization through an intermediate orthoester. The antioxidative radical scavenging activity of 1 against galvinoxyl radical, an oxyl radical, was found to be 28-fold more potent than (+)-catechin.

Regiospecific [2 + 2] photocyclodimerization of trans-4-styrylpyridines templated by cucurbit[8]uril.

Addition of HCl accelerated the photocyclodimerization of trans-4-styrylpyridine 1a in methanol and increased the yield of syn-head-to-tail (syn-HT) dimer 2a through the effect of cation-π interactions between the pyridinium ion of one molecule and the phenyl group of the other. We examined the photoirradiation products of derivatives of 1a having alkyl substituents on the phenyl group (1b-1f). The effect of the alkyl substituent on product distribution was rather limited for the photoreaction in MeOH solutions. However, the substituents had a distinct effect on the product distribution for the photoreaction of the inclusion complexes of hydrochloride salts of trans-4-styrylpyridines with cucurbit[8]uril in aqueous solutions. Introducing an alkyl group at the 2- or 3-position of the phenyl group completely shifted the major product from the syn-HT dimer to the syn-head-to-head (syn-HH) dimer. By adjusting the balance of host-guest interactions and cation-π interactions between guest molecules through systematic changes in the substituents on the phenyl ring of trans-4-styrylpyridine, we could change the orientation of the reactant molecules in the host cavity, resulting in a change of the major regioisomer of the photocyclodimerization products.

Enantiodifferentiating photocyclodimerization of 2-anthracenecarboxylic acid mediated by gamma-cyclodextrins with a flexible or rigid cap.

[reaction: see text] A series of modified gamma-cyclodextrins (CDs) with a flexible or rigid cap, synthesized and used as chiral supramolecular hosts for mediating the enantiodifferentiating photocyclodimerization of 2-anthracenecarboxylic acid, significantly improved the chemical and optical yields of chiral head-to-head cyclodimer 3, while the gamma-CD with a rigid cap dramatically inverted the stereochemical outcomes and further improved the enantioselectivities of both head-to-tail and head-to-head dimers 2 and 3.

Formation of racemic crystals of transition metal complexes by grinding 1 : 1 mixtures of enantiomeric crystals.

Grinding a 1 : 1 enantiomeric mixture of chiral transition metal complex crystals and subsequent annealing afforded crystals of a racemic compound by diffusion and rearrangement of component molecules, without melting and without racemization of each enantiomeric species.

Manganese Porphyrin Heterodimers and -trimers in Aqueous Solution.

Noncovalent face-to-face heterodimers and -trimers between beta-tetracationic and meso-tetraanionic manganese(III) porphyrins have been prepared in bulk water at pH 12. They are held together by Coulomb interactions between four beta-methylpyridinium and meso-phenylsulfonate or meso-phenylcarboxylate ion pairs in eclipsed orientations. Spectroelectrochemistry has been used to characterize the redox products and to establish reversibility. UV-visible titrations indicate quantitative trimerization at concentrations >10(-)(5) M. Cyclic voltammetry shows that all three Mn(III) ions were oxidized simultaneously to Mn(IV) at potentials close to 300 mV at pH 12. Electroreduction to Mn(II) was often not observed in the trimers, although the monomers reacted readily under the same conditions. Quantitative chemical reduction of Mn(III) to Mn(II) porphyrin trimers was, however, achieved with dithionite. Trimers containing three paramagnetic Mn(II) or Mn(IV) ions are thus easily accessible. The heterodimers and -trimers and homodimers also catalyzed the formation of dioxygen by electrooxidation of Mn(III) to Mn(IV) between 0.6 and 2.0 V while at pH 12.

Intramolecular base-accelerated radical-scavenging reaction of a planar catechin derivative bearing a lysine moiety.

A planar catechin derivative incorporating a lysine moiety was synthesized and showed approximately 400-fold increased radical-scavenging activity relative to naturally-occurring (+)-catechin.

Supramolecular photochirogenesis with biomolecules. Mechanistic studies on the enantiodifferentiation for the photocyclodimerization of 2-anthracenecarboxylate mediated by bovine serum albumin.

Photophysics and photochemistry of 2-anthracenecarboxylate (AC) bound to bovine serum albumin (BSA) were investigated in detail for the first time by electronic absorption, circular dichroism (CD), steady-state and time-resolved fluorescence, fluorescence quenching, and product analysis studies. Through the spectroscopic investigations, it was revealed that the four independent binding pockets of BSA, which are known to accommodate 1, 3, 2, and 3 AC molecules in the order of decreasing affinity, are distinctly different in hydrophobicity, chiral environment, and accessibility. Interestingly, AC bound to site 1 gave highly structured fluorescence with dual lifetimes of 4.8 and 2.1 ns in an intensity ratio of 3:2, which may be assigned to the existence of two positional or orientational isomers within the very hydrophobic site 1. In contrast, the lifetime of AC in site 2 was much longer (13.3 ns), and ACs in sites 3 and 4 have broader fluorescence spectra with lifetimes that were practically indistinguishable from that in bulk water (15.8 ns). Although each of sites 2-4 simultaneously binds multiple AC molecules, no CD exciton coupling or static fluorescence quenching was detected, indicating that ACs bound to each site are not in close proximity to each other. Quenching studies with nitromethane further confirmed the significant difference in accessibility among the binding sites; thus, ACs bound to sites 1 and 2 are highly protected from the attack of the quencher, affording 32 and 10 times smaller rate constants than that for free AC in water. Product studies in the presence and absence of nitromethane more clearly revealed the photochirogenic performance of each binding site. Although the addition of nitromethane did not greatly alter the product distribution, the enantiomeric excesses (ee's) of chiral cycloadducts 2 and 3 were critically manipulated by selectively retarding the photoreaction occurring at the more accessible binding sites. Thus, the highest ee of 38% was obtained for 2 in the presence of 18 mM nitromethane, while the highest ee of 58% was attained for 3 in the absence of nitromethane, both at [AC]/[BSA]=3.6.

Lanthanide class of a trinuclear enantiopure helical architecture containing chiral ligands: synthesis, structure, and properties.

The pinene-bipyridine carboxylic derivatives (+)- and (-)-HL, designed to form configurationally stable lanthanide complexes, proved their effectiveness as chiral building blocks for the synthesis of lanthanide-containing superstructures. Indeed a self-assembly process takes place with complete diastereoselectivity between the enantiomerically pure ligand L(-) and Ln(III) ions (La, Pr, Nd, Sm, Eu, Gd, Tb, Dy, Ho, Er), thus leading to the quantitative formation of a trinuclear supramolecular architecture with the general formula [Ln(3)(L)(6)(mu(3)-OH)(H(2)O)(3)](ClO(4))(2) (abbreviated as tris(Ln[L](2))). This class of C(3)-symmetrical compounds was structurally characterized in the solid state and solution. Electrospray (ES) mass spectrometric and (1)H NMR spectroscopic analyses indicated that the trinuclear species are maintained in solution (CH(2)Cl(2)) and are stable in the investigated concentration range (10(-2)-10(-6) m). The photophysical properties of the ligand HL and its tris(Ln[L](2)) complexes were studied at room temperature and 77 K, thus demonstrating that the metal-centered luminescence is well sensitized both for the visible and near-IR emitters. The chiroptical properties of tris(Ln[L](2)) complexes were investigated by means of circular dichroism (CD) and circularly polarized luminescence (CPL). A high CD activity is displayed in the region of pi-pi* transitions of bipyridine. CPL spectra of tris(Eu[(+)-L](2)) and tris(Tb[(+)-L](2)) present large dissymmetry factors g(em) for the sensitive transitions of Eu(III) ((5)D(0)-->(7)F(1), g(em)=-0.088) and Tb(III) ((5)D(4)-->(7)F(5), g(em)=-0.0806). The self-recognition capabilities of the system were tested in the presence of artificial enantiomeric mixtures of the ligand. (1)H NMR spectra identical to those of the enantiomerically pure complexes and investigations by CD spectroscopic analysis reveal an almost complete chiral self-recognition in the self-assembly process, thus leading to mixtures of homochiral trinuclear structures.

Pressure and temperature-controlled enantiodifferentiating [4+4] photocyclodimerization of 2-anthracenecarboxylate mediated by secondary face- and skeleton-modified gamma-cyclodextrins.

A series of secondary-face-substituted and skeleton-modified gamma-cyclodextrins (gamma-CDs) were prepared as chiral hosts for enantiodifferentiating [4+4] photocyclodimerization reactions of 2-anthracenecarboxylic acid (AC). These gamma-CD derivatives form stable ternary complexes with ACs, with altroside-bearing gamma-CDs undergoing induced-fit conformational changes upon complexation, and the photocyclodimerization of AC was, thus, dramatically accelerated. The enantiomeric excess (ee) of anti-head-to-head cyclodimer 3 was greatly enhanced in general with altroside-bearing gamma-CDs 7-9. Although mono-altro-gamma-CD 9 and 3A-azido-3A-deoxy-altro-gamma-CD 7 gave 2 in ee's smaller than those obtained with native gamma-CD, 3A-amino-3A-deoxy-altro-gamma-CD 8 yielded 2 in much higher ee's, which is likely to be ascribed to the combined effects of the less-symmetric cavity and the electrostatic interactions. The influence of temperature and high pressure on the supramolecular photochirogenic reaction has been investigated in depth. An ee as high as 71% was obtained for cyclodimer 2 in the photocyclodimerization of AC mediated by 8 at 210 MPa and -21.5 degrees C.

Electrostatic manipulation of enantiodifferentiating photocyclodimerization of 2-anthracenecarboxylate within gamma-cyclodextrin cavity through chemical modification. inverted product distribution and enhanced enantioselectivity.

In the enantiodifferentiating supramolecular photocyclodimerization of 2-anthracenecarboxylate using gamma-cyclodextrin with a dicationic side chain, a dramatic switching of the product selectivity and a significant enhancement of the enantiomeric excess were achieved by introducing a flexible dicationic sidearm to native gamma-cyclodextrin and also by lowering the temperature and solvent polarity.

Supramolecular catalysis of the enantiodifferentiating [4 + 4] photocyclodimerization of 2-anthracenecarboxylate by gamma-cyclodextrin.

2-Anthracenecarboxylic acid (AC) makes a very stable 1:2 inclusion complex with gamma-cyclodextrin (gamma-CDx) (K(1) = 161 +/- 25 M(-1), K(2) = 38 500 +/- 3300 M(-1) at 25 degrees C). The formation of the 1:2 inclusion complex accelerated the photocyclodimerization of AC. The 1:2 inclusion could be clearly verified by UV-vis, CD, and (1)H NMR spectroscopies. Although these spectroscopies provide little information about the structural isomers of the inclusion complex, there should be several structural isomers of the 1:2 inclusion complex which have a different longitudinal orientation of the guest molecules in the cavity. The isomer distribution of the photodimerization product primarily depends on the population of these orientational isomers of the 1:2 inclusion complex in the ground state before photoreaction, because, in the lifetime of the excited singlet state, exchanging the orientation is impossible. The enantioselectivity of the photodimerization originates from the difference in the stability of the diastereomeric pair of orientational isomers of the 1:2 inclusion complex in the ground state, which are the precursors of the enantiomers of a specific chiral cyclodimer. The ee of a chiral cyclodimer 2 was 32% at 25 degrees C and was enhanced by lowering the temperature to 41% at 0 degrees C. This is the highest value reported for the asymmetric photodimerization in solution.

Bovine serum albumin-mediated enantiodifferentiating photocyclodimerization of 2-anthracenecarboxylate.

Enantiodifferentiating photocyclodimerization of 2-anthracenecarboxyalate (AC) was performed at 25 degrees C in aqueous buffer solution (pH 7) in the presence of bovine-serum albumin (BSA) to afford four [4 + 4] cyclodimers, i.e., anti- and syn-head-to-tail (HT) (1 and 2) and anti- and syn-head-to-head (HH) dimers (3 and 4), of which only 2 and 3 are chiral. We found that (1) BSA possesses four sets of binding sites for AC of different affinities, stoichiometries, and chiral environment for photoreaction, which bind 1, 3, 2, and 3 AC molecules with binding constants of 5.3 x 107, 1.3 x 105, 1.4 x 104, and 3.0 x 103 M-1, respectively, (2) the regioselectivity of photodimerization is switched from HT to HH by adding BSA (the HH/HT ratio varies from 0.28 to 4.3), (3) BSA-mediated photodimerization of AC affords optically active products 2 and 3 of up to 29% and 41% ee, respectively. It is emphasized that the selective excitation of bound substrate, utilizing the spectral shift upon complexation with BSA, is not a prerequisite for efficient photochirogenesis using biomolecules.

Pressure control of enantiodifferentiating photoisomerization of cyclooctenes sensitized by chiral benzenepolycarboxylates. The origin of discontinuous pressure dependence of the optical yield.

Pressure effects on enantiodifferentiating geometrical photoisomerizations of (Z)-cyclooctene and (Z,Z)-cycloocta-1,5-diene sensitized by chiral benzene-1,2,4,5-tetracarboxylate were investigated over a pressure range of 0.1-750 MPa. Enantiomeric excesses (ee's) of the (E)- and (E.Z)-isomers obtained displayed discontinuous pressure dependencies, affording distinctly different differential activation volumes (delta delta V++) for each range, indicating alteration of the enantiodifferentiation mechanism. The switching of delta delta V++ occurred at essentially the same pressures of 200 and 400 MPa, which are shared by all the chiral sensitizers, irrespective of the chiral auxiliary employed. Circular dichroism spectral examinations at pressures of up to 400 MPa also revealed that the chiral sensitizers undergo discontinuous conformational changes at 200 MPa, which most likely lead to switching of the enantiodifferentiating sensitization mechanism in the exciplex intermediate.

Heterodimerization of dye-modified cyclodextrins with native cyclodextrins.

The heterodimerization behavior of dye-modified beta-cyclodextrins (1-6) with native cyclodextrins (CDs) was investigated by means of absorption and induced circular dichroism spectroscopy in an aqueous solution. Three types of azo dye-modified beta-CDs (1-3) show different association behaviors, depending on the positional difference and the electronic character of substituent connected to the CD unit in the dye moiety. p-Methyl red-modified beta-CD (1), which has a 4-(dimethylamino)azobenzene moiety connected to the CD unit at the 4' position by an amido linkage, forms an intramolecular self-complex, inserting the dye moiety in its beta-CD cavity. It also associates with the native alpha-CD by inserting the moiety of 1 into the alpha-CD cavity. The association constants for such heterodimerization are 198 M(-1) at pH 1.00 and 305 M(-1) at pH 6.59, which are larger than the association constant of 1 for beta-CD (43 M(-1) at pH 1.00). Methyl red-modified 2, which has the same dye moiety as that for 1 although its substituent position is different from that of 1, does not associate even with alpha-CD due to the stable self-intramolecular complex, in which the dye moiety is deeply included in its own cavity of beta-CD. Alizarin yellow-modified CD (3), which has an azo dye moiety different from that of 1 and 2, caused a slight spectral variation upon addition of alpha-CD, suggesting that the interaction between 3 and alpha-CD is weak. On the other hand, phenolphthalein-modified beta-CD (4), which forms an intermolecular association complex in its higher concentrations, binds with beta-CD with an association constant of 787 M(-1) at pH 10.80, where 4 exists as the dianion monomer in the absence of beta-CD. p-Nitorophenol-modified beta-CDs (5 and 6), each having p-nitorophenol moieties with a different connecting part with an amido and amidophenyl group, respectively, associated with alpha-CD with association constants of 66 and 16 M(-1) for 5 and 6, respectively. The phenyl unit in the connecting part of 6 may prevent the smooth binding with alpha-CD. All these results suggest that the dye-modified CDs, in which the dye part is not tightly included in its CD cavity, associate with the native CD to form heterodimer composed of two different CD units by inserting the dye moiety into the native CD unit. The resulting heterodimers have a cavity that can bind another appending moiety of host molecules. On this basis, more ordered molecular arrays or the supramolecular hereropolymers can be constructed.