Radial Hetero[5]catenanes: Peripheral Isomer Sequences of the Interlocked Macrocycles

A pair of radial [5]catenanes, with either an isomeric cyclic ‐AABB‐ or ‐ABAB‐ type sequence of the interlocked β‐cyclodextrin (β‐CD) and cucurbit[6]uril (CB[6]) units, has been efficiently synthesized. Because of a marked difference in the binding strength and interlocking sequence of the peripheral macrocycles, interesting sequence‐dependent properties, characteristic of mechanically bonded macrocycles, were realized. Variable‐temperature ¹H NMR studies showed that the ‐ABAB‐ isomer has a more independent β‐CD dynamic, whereas the β‐CD motions in the ‐AABB‐ isomer are coupled. Dynamics of the pH‐insensitive β‐CD can also be further modulated upon base‐triggered mobilization of the CB[6]. These unique properties of the mechanical bond expressed in a sequence‐specific fashion and the transmission of the control on the macrocycle dynamics from one interlocked component to another, highlight the potential of similar complex hetero[n]catenanes in the design of advanced, multicomponent molecular machines.     

The Assembly of Macrocyclic Bis‐ and Tetra‐β‐lactams with Embedded Platinum or Palladium Square‐Planar Centers

The synthesis, isolation, and full characterization of different types of stable, metal‐assembled macrocyclic β‐lactams are reported. By using adequately functionalized bis‐β‐lactams with defined stereochemistry as building blocks, a series of mono‐ and bimetallic Pd and Pt macrocycles has been prepared in good to quantitative yields. These novel structures combine the β‐lactam moiety with transition‐metal fragments with cis‐square‐planar geometry and constitute a new class of metal‐assembled cavities involving molecules with biological relevance as building blocks. By combining the adequate ligands, metallic fragments, and tuning the reaction conditions, different mono‐ and bimetallic macrocyclic β‐lactam cavities can be selectively obtained. Macrocycles with Pt–ethynyl groups are suitable to form host–silver triflate guest complexes in a tweezer fashion.     

Internal Nucleophilic Catalyst Mediated Cyclisation/Ring Expansion Cascades for the Synthesis of Medium‐Sized Lactones and Lactams

A strategy for the synthesis of medium‐sized lactones and lactams from linear precursors is described in which an amine acts as an internal nucleophilic catalyst to facilitate a novel cyclisation/ring expansion cascade sequence. This method obviates the need for the high‐dilution conditions usually associated with medium‐ring cyclisation protocols, as the reactions operate exclusively via kinetically favourable “normal”‐sized cyclic transition states. This same feature also enables biaryl‐containing medium‐sized rings to be prepared with complete atroposelectivity by point‐to‐axial chirality transfer.     

Synthesis of phosphocyclic 2,2′,7,7′-tetrahydroxydinaphthylmethane derivatives

Two types of phosphocyclic derivatives were synthesized by phosphorylation of 2,2′,7,7′-tetrahydroxydinaphthylmethane with triamidophosphites: triphosphorus containing compounds with a phosphocine ring and two acyclic diamidophosphite fragments, and tetraphosphorus-containing macrocycles with a 24-membered ring and two eight-membered phosphorus rings. It was shown that interaction of triphosphorus compounds with resorcinarene gives tetraphosphorus macrocycles.     

Reversible Redox Reaction Between Antiaromatic and Aromatic States of 32π‐Expanded Isophlorins

32π‐antiaromatic expanded isophlorins with a varying number of thiophene and furan rings adopt either planar, ring‐inverted, or twisted conformations depending on the number of furan rings in the macrocycle. However, they exhibit identical reactivity with respect to their oxidation to aromatic 30π‐dicationic species under acidic conditions. These 32π‐antiaromatic macrocycles can also be oxidized with [Et₃O⁺SbCl₆^?]and NOBF₄ to generate dications, thus confirming ring oxidation of macrocycles. Furthermore, they can be reduced back to their parent 32π‐antiaromatic state by triethylamine, Zn, or FeCl₂. Single‐crystal X‐ray diffraction analysis confirmed a figure‐eight conformation for a hexafuran system, which opens to a planar structure upon oxidation.     

Synthesis and ring‐opening polymerization of macrocyclic (arylene thioether ketone) oligomers

Macrocyclic (arylene thioether ketone) oligomers together with a linear poly(phenylene sulfide ketone) oligomer were synthesized by a one‐step reaction. The macrocycles and linear oligomer were fully characterized by ¹³C‐NMR, H‐NMR, matrix assisted laser desorption/ionization time‐of‐flight mass spectrometry (MALDI‐TOF‐MS), differential scanning calorimetry (DSC) and FT‐IR. Uncatalyzed, simultaneously ring‐opening polymerization (ROP) of the macrocycles and the mixture of macrocycles and linear oligomer were carried out under dynamic heating conditions. The ROP temperature of the macrocycles decreased upon mixing it with the linear oligomer. The ROP conditions and mechanism were investigated and discussed. The macrocycles and their mixture show potential applications in high temperature adhesives and sealants. Copyright © 2006 John Wiley & Sons, Ltd.     

12‐ to 22‐Membered Bridged β‐Lactams as Potential Penicillin‐Binding Protein Inhibitors

As potential inhibitors of penicillin‐binding proteins (PBPs), we focused our research on the synthesis of non‐traditional 1,3‐bridged β‐lactams embedded into macrocycles. We synthesized 12‐ to 22‐membered bicyclic β‐lactams by the ring‐closing metathesis (RCM) of bis‐ω‐alkenyl‐3(S)‐aminoazetidinone precursors. The reactivity of 1,3‐bridged β‐lactams was estimated by the determination of the energy barrier of a concerted nucleophilic attack and lactam ring‐opening process by using ab initio calculations. The results predicted that 16‐membered cycles should be more reactive. Biochemical evaluations against R39 DD‐peptidase and two resistant PBPs, namely, PBP2a and PBP5, revealed the inhibition effect of compound 4d , which featured a 16‐membered bridge and the N‐tert‐butyloxycarbonyl chain at the C3 position of the β‐lactam ring. Surprisingly, the corresponding bicycle, 12d , with the PhOCH₂CO side chain at C3 was inactive. Reaction models of the R39 active site gave a new insight into the geometric requirements of the conformation of potential ligands and their steric hindrance; this could help in the design of new compounds.     

N‐(p‐Chloro­phenyl)‐3,3‐di­phenyl‐4‐(β‐phenyl­styryl)azetidin‐2‐one

In the title compound, C₃₅H₂₆ClNO, the four‐membered β‐lactam ring is essentially planar, with a maximum deviation of 0.012 (1) Å for the N atom. The C—C bond lengths in the β‐lactam ring are 1.591 (2) and 1.549 (2) Å. The two phenyl rings attached to the β‐lactam ring are nearly perpendicular to each other [83.2 (1)°].     

Ring‐opening polycondensations

Ring‐opening polycondensation is a novel synthetic strategy using heterocycles of any ring size having two reactive bonds as bifunctional monomers in step‐growth polymerizations. The first part of this article reviews previous publications. The previous studies mainly dealt with syntheses of polyesters from tin‐containing macrocycles including cyclic polylactones. These tin‐containing cyclic oligomers or polymers were easily obtained in two ways, either by ring‐closing polycondensation of dibutyltin compounds with preformed diols or by ring‐expansion polymerizations of lactones by means of cyclic tin‐initiators. The second part of this article presents new results which deal with ring‐opening polycondensations of silicon containing macrocycles derived from oligo(ethylene glycol)s. In these cases the chain growth proceeds by elimination of dimethyl dichlorosilane. In addition to syntheses of homopolyesters, copolycondensations with silylated or stanylenated monomers were studied. Finally, the thermodynamical aspects of ring‐opening polycondensations will be discussed.     

Defying entropy: forming large head-to-tail macrocycles in the gas phase

Spectral fingerprints: Collision-induced dissociation (CID) of protonated peptides in the gas phase results in linear fragment ions with a five-membered oxazolone ring on their C-terminal side. Infrared spectroscopy confirms that smaller fragments adopt oxazolone structures. Conversely, in mid-sized and larger fragments an isomerization to "head-to-tail" macrocycles is observed (see picture).     

Mass spectrometric study of oligourea macrocycles and their anion binding behavior

Two series, one of tris‐urea macrocycles and another of hexakis‐urea macrocycles, are examined by (tandem) Fourier‐transform ion cyclotron resonance (FTICR) mass spectrometry with respect to their fragmentation patterns and anion binding properties. All macrocycles are based on two different building blocks, one of which is a very rigid xanthene unit and the other one is a more flexible diphenyl ether. The composition and the sequence of these units thus determine their flexibility. During the fragmentation of deprotonated oligourea macrocycles in the gas phase, one urea N? CO bond is cleaved followed by a scrambling reaction within the macrocycle structure. Consequently, fragments are observed that deviate from those that would be expected from the sequence of the subunits. Interesting anion binding properties involve the simultaneous recognition of two chloride anions by one of the hexakis‐urea macrocycles, whose flexibility allows this host to form a double‐helical structure. Flexibility also determines which of the hexameric receptors bears a high sulfate affinity. The interaction energy between some of the macrocycles and sulfate is high enough to even stabilize the intrinsically unstable sulfate dianion. Copyright © 2009 John Wiley & Sons, Ltd.     

Coordination assembled rings of ferrocene-bridged trisporphyrin with flexible hinge-like motion: selective dimer ring formation, its transformation to larger rings, and vice versa

Ferrocene-bridged trisporphyrin (2) was synthesized by two-steps condensation of corresponding aldehydes and dipyrromethanes, and its self-assembling behavior based on the complementary coordination motif of imidazolylporphyrinatozinc(II) was investigated in conjunction with hinge-like flexibility given by freely rotating cyclopentadienyl rings of ferrocene connector. Ferrocene-bridged trisporphyrin (2) spontaneously and exclusively generated the dimeric ring (7) upon simple zinc(II) insertion, indicating that the freely rotating hinge connector favored the smallest ring formation. Taking advantage of the unique hinge-like flexibility of ferrocene, we attempted to transform the dimer ring into a mixture of porphyrin macrocycles by reorganizing the structure cleaved once by pyridine. A series of porphyrin macrocycles from trimer to decamer can be separated into its components by preparative gel permeation chromatograms. Macrocycles obtained are kept stable in the absence of coordinating solvents. On the other hand, they were easily transformed to the dimer ring in the presence of coordinating solvents such as methanol, showing that the transformation is completely reversible and can be controlled by the choice of the solvent system. A series of porphyrin macrocycles was confirmed via covalent linking of each complementary coordination dimer pair by metathesis reaction in the presence of Grubbs's catalyst. The coordination behavior of the bidentate ligands with different spacer lengths toward the dimer ring revealed that only the bidentate ligand (15) with a spacer length that matched the facing central porphyrins was selectively accommodated inside the ring. Coordination assembled flexible rings with tunable cavities and multiple coordination sites will be used as versatile hosts for a wide variety of guest molecules.     

Substrate‐Induced Dimerization Assembly of Chiral Macrocycle Catalysts toward Cooperative Asymmetric Catalysis

An artificial system of substrate‐induced dimerization assembly of chiral macrocycle catalysts enables a highly cooperative hydrogen‐bonding activation network for efficient enantioselective transformation. These macrocycles contain two thiourea and two chiral diamine moieties and dimerize with sulfate to form a sandwich‐like assembly. The macrocycles then adopt an extended conformation and reciprocally complement the hydrogen‐bonding interaction sites. Inspired by the guest‐induced dynamic assembly, these macrocycles catalyze the decarboxylative Mannich reaction of cyclic aldimines containing a sulfamate heading group. The imine substrate can be activated toward nucleophilic attack of β‐ketoacid by a cooperative hydrogen‐bonding network enabled by sulfamate‐induced dimerization assembly of the macrocycle catalysts. Highly efficient (>95 % yield in most cases) and enantioselective (up to 97.5:2.5 er) transformation of a variety of substrates using only 5 mol % macrocycle was achieved.     

Cycling a Tether into Multiple Rings: Pt-Bridged Macrocycles for Differentiated Guest Recognition,Pseudorotaxane Transformations,and Guest Capture and Release

Macrocycle engineering is a key topic in supramolecular chemistry. When synthesizing a ring, one can obtain either complex mixtures of macrocycles of different sizes or a single ring if a template is utilized. Here, we unite these approaches along with post-synthetic modifications to transform a single tether into multiple rings—up to five per tether. The macrocycles contain two bridged phenylpyridine ligands that are connected through a Pt atom, which defines the rings’ shape, size, and host activity. All rings undergo redox reactions (between Pt^II and Pt^IV) that allow for large conformational changes. Their reactivity, together with their host performance, is a convenient way to control the capture and release of guests, to mediate ring transformations, and to control pseudorotaxane-to-pseudorotaxane conversions. This novel approach could serve to assemble other libraries of small ring molecules, create cyclic polymers bridged by responsive-at-metal nodes, and produce processable mechanically interlocked molecules.     

Designable Aluminum Molecular Rings: Ring Expansion and Ligand Functionalization

Presented herein are the Al^III molecular ring architectures from 8‐ring to 16‐ring. Although there are numerous reported cyclic coordination compounds based on transition metals, gallium, or lanthanides, the Al versions are less developed due to the fast hydrolysis nature of Al³⁺ ion. With the assistant of monohydric alcohols, a series of atomic precisely Al molecular rings based on benzoates are synthesized. The ring expansion of these Al‐rings from 8‐ring to 16‐ring is related to the monohydric alcohol structure‐directing agents. Moreover, the organic ligands on the Al‐rings can be modified by using various benzoate derivatives, which lead to tunable surface properties of the Al‐rings from hydrophilicity to ultra‐hydrophobicity. Importantly, 4‐aminobenzoic acid bridged 16‐ring is soluble in organic solvents and exhibits high solution stability revealed by mass spectroscopy. Ligand substitution also can be performed between these Al‐rings, which reveal controllable ligand functionalization of these Al‐rings.     

Polylactones, 56. ABA Triblock Copolymers Derived from ε‐Caprolactone or L‐Lactide and a Central Polysiloxane Block

A commercial oligosiloxane having two γ‐hydroxypropyl endgroups and a number‐average molecular weight (M̄_n) around 1 000 Da was condensed with Bu₂Sn(OMe)₂ yielding tin‐containing macrocycles but no polymers. These macrocycles reacted with γ‐thiobutyrolactone by insertion of one thiolactone per Sn—O bond. When ε‐caprolactone was added a ring‐expansion polymerization was initiated, so that the M̄_n could be controlled via the monomer/initiator (M/I) ratio. Triblock copolymers with free OH endgroups were obtained by removal of the Bu₂Sn group from the cyclic polymers with 1,2‐dimercaptoethane or methanol. Analogous cyclic and linear triblockcopolymers were prepared from L ‐lactide.     

Radical‐Mediated 1,2‐Formyl/Carbonyl Functionalization of Alkenes and Application to the Construction of Medium‐Sized Rings

A novel radical 1,2‐formylfunctionalization of alkenes involving 1,2(4,5)‐formyl migration triggered by addition of various carbon‐ and heteroatom‐centered radicals to alkenes has been developed for the first time, thus providing straightforward access to diverse β‐functionalized aldehydes with good efficiency, remarkable selectivity, and excellent functional group tolerance. Analogous transformations mediated by a keto‐carbonyl migration have also been effected under similar conditions. This method was used to access ring systems including various benzannulated nine‐, ten‐, and eleven‐membered rings, complex 6‐5(6,7)‐6(5) fused rings, and bridged rings with diverse functionalities.     

Self‐diffusion coefficient of ring polymers in semidilute solution

In a topologically constraining environment the size of a flexible nonconcatenated ring polymer (macrocycles) and its dynamics are known to differ from that of linear polymers. Hence, the diffusion coefficient of ring polymers can be expected to be different from linear chains. We present here scaling arguments for the concentration and molecular weight dependence of self‐diffusion coefficient of ring polymers in semidilute solutions, and show that contrary to expectations these scaling relations are identical to what is known for linear polymers. At higher concentrations excluded volume interactions arising from possibilities of segmental overlap can become effective for large ring polymers. In this regime the diffusion coefficient of large ring polymers shows a relatively weaker dependence on concentration and molecular weight. ©2008 Wiley Periodicals, Inc. J Polym Sci Part B: Polym Phys 46: 2370–2379, 2008     

Carbamoyl Radical‐Mediated Synthesis and Semipinacol Rearrangement of β‐Lactam Diols

In an approach to the biologically important 6‐azabicyclo[3.2.1]octane ring system, the scope of the tandem 4‐exo‐trig carbamoyl radical cyclization—dithiocarbamate group transfer reaction to ring‐fused β‐lactams is evaluated. β‐Lactams fused to five‐, six‐, and seven‐membered rings are prepared in good to excellent yield, and with moderate to complete control at the newly formed dithiocarbamate stereocentre. No cyclization is observed with an additional methyl substituent on the terminus of the double bond. Elimination of the dithiocarbamate group gives α,β‐ or β,γ‐unsaturated lactams depending on both the methodology employed (base‐mediated or thermal) and the nature of the carbocycle fused to the β‐lactam. Fused β‐lactam diols, obtained from catalytic OsO₄‐mediated dihydroxylation of α,β‐unsaturated β‐lactams, undergo semipinacol rearrangement via the corresponding cyclic sulfite or phosphorane to give keto‐bridged bicyclic amides by exclusive N‐acyl group migration. A monocyclic β‐lactam diol undergoes Appel reaction at a primary alcohol in preference to semipinacol rearrangement. Preliminary investigations into the chemo‐ and stereoselective manipulation of the two carbonyl groups present in a representative 7,8‐dioxo‐6‐azabicyclo[3.2.1]octane rearrangement product are also reported.     

Regiodirected phosphorylation of 2,2′,7,7′-tetrahydroxydinaphthylmethane

The phosphorylation of 2,2′,7,7′-tetrahydroxydinaphthylmethane was studied and the influence of molecule pre-organization on the regioselectivity of functionalization was investigated. The reactions of 2,2′,7,7′-tetrahydroxydinaphthylmethane with phosphorous amides containing 1-3 amide bonds gave oligophosphorylated derivatives differing in the number and the nature of phosphorus fragments and in the size of phosphorus rings: tetraphosphorus macrocycles containing one 24-membered and two eight-membered phosphorus rings, triphosphorus compounds containing a phosphocine ring and two acyclic phosphorus fragments, and tetraphosphorylated derivatives with four phosphorus groups in the molecule. The possibility of controlling the regioselectivity of phosphorylation by using reagents differing in the number and activity of P-N bonds was demonstrated.