Formation of Trinuclear Rhodium‐Hydride Complexes [{Rh(PP*)H}3‐ (μ2‐H)3(μ3‐H)][anion]2—During Asymmetric Hydrogenation?

Recently described and fully characterized trinuclear rhodium‐hydride complexes [{Rh(PP*)H}₃(μ₂‐H)₃(μ₃‐H)][anion]₂ have been investigated with respect to their formation and role under the conditions of asymmetric hydrogenation. Catalyst–substrate complexes with mac (methyl (Z)‐ N‐acetylaminocinnamate) ([Rh(tBu‐BisP*)(mac)]BF₄, [Rh(Tangphos)(mac)]BF₄, [Rh(Me‐BPE)(mac)]BF₄, [Rh(DCPE)(mac)]BF₄, [Rh(DCPB)(mac)]BF₄), as well as rhodium‐hydride species, both mono‐([Rh(Tangphos)‐ H₂(MeOH)₂]BF₄, [Rh(Me‐BPE)H₂(MeOH)₂]BF₄), and dinuclear ([{Rh(DCPE)H}₂(μ₂‐H)₃]BF₄, [{Rh(DCPB)H}₂(μ₂‐H)₃]BF₄), are described. A plausible reaction sequence for the formation of the trinuclear rhodium‐hydride complexes is discussed. Evidence is provided that the presence of multinuclear rhodium‐hydride complexes should be taken into account when discussing the mechanism of rhodium‐promoted asymmetric hydrogenation.     

C?H/π‐Interaction‐Guided Self‐Assembly in π‐Conjugated Oligomers

We report CH/π hydrogen‐bond‐driven self‐assembly in π‐conjugated skeletons based on oligophenylenevinylenes (OPVs) and trace the origin of interactions at the molecular level by using single‐crystal structures. OPVs were designed with appropriate pendants in the aromatic core and varied by hydrocarbon or fluorocarbon tails along the molecular axis. The roles of aromatic π‐stack, van der Waals forces, fluorophobic effect and CH/π interactions were investigated on the theromotropic liquid crystallinity of OPV molecules. Single‐crystal structures of hydrocarbon OPVs provided direct evidence for the existence of CH/π interactions between the π‐ring (H‐bond acceptor) and alkyl C? H (H‐bond donor). The four important crystallographic parameters, d_c?x=3.79 Å, θ=21.49°, φ=150.25° and d_Hp?x=0.73 Å, matched in accordance with typical CH/π interactions. The CH/π interactions facilitate the close‐packing of mesogens in x–y planes, which were further protruded along the c axis producing a lamellar structure. In the absence of CH/π interactions, van der Waals interactions drove the assembly towards a Schlieren nematic texture. Fluorocarbon OPVs exhibited smectic liquid‐crystalline textures that further underwent Smectic A (SmA) to Smectic C (SmC) phase transitions with shrinkage up to 11 %. The orientation and translational ordering of mesogens in the liquid‐crystalline (LC) phases induced H‐ and J‐type molecular arrangements in fluorocarbon and hydrocarbon OPVs, respectively. Upon photoexcitation, the H‐ and J‐type molecular arrangements were found to emit a blue or yellowish/green colour. Time‐resolved fluorescence decay measurements confirmed longer lifetimes for H‐type smectic OPVs relative to that of loosely packed one‐dimensional nematic hydrocarbon‐tailed OPVs.     

Synthesis of Perfluoroalkyl‐Substituted γ‐Lactones and 4,5‐Dihydropyridazin‐3(2H)‐ones via Donor?Acceptor Cyclopropanes

Rh₂(OAc)₄‐Catalyzed decomposition of diazo esters in the presence of perfluoroalkyl‐ or perfluoroaryl‐substituted silyl enol ethers smoothly provided the corresponding alkyl 2‐siloxycyclopropanecarboxylates in very good yields. The generated donor? acceptor cyclopropanes are equivalents of γ‐oxo esters, which we demonstrated by their one‐pot transformations to yield fluorine‐containing heterocycles. A reductive procedure selectively afforded perfluoroalkyl‐substituted γ‐hydroxy esters or γ‐lactones. The treatment of the donor? acceptor cyclopropanes with hydrazine or phenylhydrazine afforded a series of perfluoroalkyl‐ and perfluoroaryl‐substituted 4,5‐dihydropyridazin‐3(2H)‐ones.     

Rhodium‐catalyzed coupling reactions of β‐ or α,β‐substituted vinylpyridines with alkenes via C?H bond activation

β‐ or α,β‐Substituted vinylpyridines react with 3,3‐dimethylbut‐1‐ene in the presence of Wilkinson catalyst [RhCl(PPh₃)₃] to give the corresponding alkylated products along with unusually isomerized products. © 2002 Wiley Periodicals, Inc. Heteroatom Chem 13:346–350, 2002; Published online in Wiley Interscience (www.interscience.wiley.com). DOI 10.1002/hc.10045     

Enantioselective Palladium‐Catalyzed Insertion of α‐Aryl‐α‐diazoacetates into the O?H Bonds of Phenols

A palladium‐catalyzed asymmetric O H insertion reaction was developed. Palladium complexes with chiral spiro bisoxazoline ligands promoted the insertion of α‐aryl‐α‐diazoacetates into the O H bond of phenols with high yield and excellent enantioselectivity under mild reaction conditions. This palladium‐catalyzed asymmetric O H insertion reaction provided an efficient and highly enantioselective method for the preparation of synthetically useful optically active α‐aryl‐α‐aryloxyacetates.     

Electrophilic Arene Hydroxylation and Phenol O?H Oxidations Performed by an Unsymmetric μ‐η1:η1‐O2‐Peroxo Dicopper(II) Complex

Reactions of the unsymmetric dicopper(II) peroxide complex [Cu^II₂(μ‐η¹:η¹‐O₂)(m‐XYL^N3N4)]²⁺ ( 1 O₂ , where m‐XYL is a heptadentate N‐based ligand), with phenolates and phenols are described. Complex 1 O₂ reacts with p‐X‐PhONa (X=MeO, Cl, H, or Me) at ?90 °C performing tyrosinase‐like ortho‐hydroxylation of the aromatic ring to afford the corresponding catechol products. Mechanistic studies demonstrate that reactions occur through initial reversible formation of metastable association complexes [Cu^II₂(μ‐η¹:η¹‐O₂)(p‐X‐PhO)(m‐XYL^N3N4)]⁺ ( 1 O₂ ?X‐PhO) that then undergo ortho‐hydroxylation of the aromatic ring by the peroxide moiety. Complex 1 O₂ also reacts with 4‐X‐substituted phenols p‐X‐PhOH (X=MeO, Me, F, H, or Cl) and with 2,4‐di‐tert‐butylphenol at ?90 °C causing rapid decay of 1 O₂ and affording biphenol coupling products, which is indicative that reactions occur through formation of phenoxyl radicals that then undergo radical C? C coupling. Spectroscopic UV/Vis monitoring and kinetic analysis show that reactions take place through reversible formation of ground‐state association complexes [Cu^II₂(μ‐η¹:η¹‐O₂)(X‐PhOH)(m‐XYL^N3N4)]²⁺ ( 1 O₂ ?X‐PhOH) that then evolve through an irreversible rate‐determining step. Mechanistic studies indicate that 1 O₂ reacts with phenols through initial phenol binding to the Cu₂O₂ core, followed by a proton‐coupled electron transfer (PCET) at the rate‐determining step. Results disclosed in this work provide experimental evidence that the unsymmetric 1 O₂ complex can mediate electrophilic arene hydroxylation and PCET reactions commonly associated with electrophilic Cu₂O₂ cores, and strongly suggest that the ability to form substrate?Cu₂O₂ association complexes may provide paths to overcome the inherent reactivity of the O₂‐binding mode. This work provides experimental evidence that the presence of a H⁺ completely determines the fate of the association complex [Cu^II₂(μ‐η¹:η¹‐O₂)(X‐PhO(H))(m‐XYL^N3N4)]ⁿ⁺ between a PCET and an arene hydroxylation reaction, and may provide clues to help understand enzymatic reactions at dicopper sites.     

Is Cyclopropane Really the σ‐Aromatic Paradigm?

Dewar proposed the σ‐aromaticity concept to explain the seemingly anomalous energetic and magnetic behavior of cyclopropane in 1979. While a detailed, but indirect energetic evaluation in 1986 raised doubts—“There is no need to involve ‘σ‐aromaticity’,”—other analyses, also indirect, resulted in wide‐ranging estimates of the σ‐aromatic stabilization energy. Moreover, the aromatic character of “in‐plane”, “double”, and cyclically delocalized σ‐electron systems now seems well established in many types of molecules. Nevertheless, the most recent analysis of the magnetic properties of cyclopropane (S. Pelloni, P. Lazzeretti, R. Zanasi, J. Phys. Chem. A 2007 , 111, 8163–8169) challenged the existence of an induced σ‐ring current, and provided alternative explanations for the abnormal magnetic behavior. Likewise, the present study, which evaluates the σ‐aromatic stabilization of cyclopropane directly for the first time, fails to find evidence for a significant energetic effect. According to ab initio valence bond (VB) computations at the VBSCF/cc‐PVTZ level, the σ‐aromatic stabilization energy of cyclopropane is, at most, 3.5 kcal mol^?1 relative to propane, and is close to zero when n‐butane is used as reference. Trisilacyclopropane also has very little σ‐aromatic stabilization, compared to Si₃H₈ (6.3 kcal mol^?1) and Si₄H₁₀ (4.2 kcal mol^?1). Alternative interpretations of the energetic behavior of cyclopropane (and of cyclobutane, as well as their silicon counterparts) are supported.     

Note: Helix or No Helix of β‐Peptides Containing β3hAla(αF) Residues?

A remote ⁴J(F,H) coupling (F? C(α)? C(O)? N? H) of up to 4.2 Hz in α‐fluoro amides with antiperiplanar arrangement of the C? F and the C?O bonds (dihedral angle F? C? C?O ca. 180°) confirms that previous NMR determinations, using the XPLOR‐NIH procedure, of the secondary structures of β‐peptides containing β³hAla(αF) and β³hAla(αF₂) residues were correct. In contrast, molecular‐dynamics (MD) simulations, using the GROMOS program with the 45A3 force field, led to an incorrect conclusion about the relative stability of secondary structures of these β‐peptides. The problems encountered in NMR analyses and computations of the structures of backbone‐F‐substituted peptides are briefly discussed.     

Evaluation of Electron Population Terms for 〈rSe−3〉4p, 〈rS−3〉3p,and 〈rO−3〉2p: How Do HOMO and LUMO Shrink or Expand Depending on Nuclear Charges?

Electron population terms are evaluated for N=Se, S, and O. Calculations are performed on HOMO and LUMO constructed by pure atomic 4p(Se), 3p(S), and 2p(O) orbitals, employing the 6-311+G(3d) and/or 6-311(++)G(3df,3pd) basis sets at the HF, MP2, and DFT (B3 LYP) levels. Se(4+), Se(2+), Se(0), and Se(2-) with the O(h) symmetry are called G(A: Se) and HSe(+), H(2)Se, and HSe(-) with the C(infinityh) or C(2v) symmetry are named G(B: Se), here [G(A+B: Se) in all]. HOMO and LUMO in G(A+B: N) (N=Se, S, and O) satisfy the conditions of the calculations for . The (4p), (3p), and (2p) values correlate well with the corresponding MO energies (epsilon(N)) for all calculation levels employed. Plots of (HOMO) and (LUMO) versus Q(N) (N=Se, S, and O) at the HF and MP2 levels are analyzed as two correlations. However, the plots at the DFT level can be analyzed as single correlation. A regression curve is assumed for the analysis. Behaviors of clarify how valence orbitals shrink or expand depending on Q(N). The applicability of is examined to establish a new method that enables us to analyze chemical shifts with the charge effect separately from others. A utility program derived from the Gaussian 03 (NMRANAL-NH03G) is applied to evaluate and examine the applicability to the NMR analysis.     

Access to β‐Lactams by Enantioselective Palladium(0)‐Catalyzed C(sp3)?H Alkylation

β‐Lactams are very important structural motifs because of their broad biological activities as well as their propensity to engage in ring‐opening reactions. Transition‐metal‐catalyzed C H functionalizations have emerged as strategy enabling yet uncommon highly efficient disconnections. In contrast to the significant progress of Pd⁰‐catalyzed C H functionalization for aryl–aryl couplings, related reactions involving the formation of saturated C(sp³) C(sp³) bonds are elusive. Reported here is an asymmetric C H functionalization approach to β‐lactams using readily accessible chloroacetamide substrates. Important aspects of this transformation are challenging C(sp³) C(sp³) and strain‐building reductive eliminations to for the four‐membered ring. In general, the β‐lactams are formed in excellent yields and enantioselectivities using a bulky taddol phosphoramidite ligand in combination with adamantyl carboxylic acid as cocatalyst.     

Is the μ‐Oxo‐μ‐Peroxodiiron Intermediate of a Ribonucleotide Reductase Biomimetic a Possible Oxidant of Epoxidation Reactions?

Density functional calculations on a mu-oxo-mu-peroxodiiron complex (1) with a tetrapodal ligand BPP (BPP=N,N-bis(2-pyridylmethyl)-3-aminopropionate) are presented that is a biomimetic of the active site region of ribonucleotide reductase (RNR). We have studied all low-lying electronic states and show that it has close-lying broken-shell singlet and undecaplet (S=0, 5) ground states with essentially two sextet spin iron atoms. In strongly distorted electronic systems in which the two iron atoms have different spin states, the peroxo group moves considerably out of the plane of the mu-oxodiiron group due to orbital rearrangements. The calculated absorption spectra of (1,11)1 are in good agreement with experimental studies on biomimetics and RNR enzyme systems. Moreover, vibrational shifts in the spectrum due to (18)O(2) substitution of the oxygen atoms in the peroxo group follow similar trends as experimental observations. To identify whether the mu-oxo-mu-1,2-peroxodiiron or the mu-oxo-mu-1,1-peroxodiiron complexes are able to epoxidize substrates, we studied the reactivity patterns versus propene. Generally, the reactions are stepwise via radical intermediates and proceed by two-state reactivity patterns on competing singlet and undecaplet spin state surfaces. However, both the mu-oxo-mu-1,2-peroxodiiron and mu-oxo-mu-1,1-peroxodiiron complex are sluggish oxidants with high epoxidation barriers. The epoxidation barriers for the mu-oxo-mu-1,1-peroxodiiron complex are significantly lower than the ones for the mu-oxo-mu-1,2-peroxodiiron complex but still are too high to be considered for catalytic properties. Thus, theory has ruled out two possible peroxodiiron catalysts as oxidants in RNR enzymes and biomimetics and the quest to find the actual oxidant in the enzyme mechanism continues.     

Easily Accessible Auxiliary for Palladium‐Catalyzed Intramolecular Amination of C(sp2)?H and C(sp3)?H Bonds at δ‐ and ε‐Positions

An easily synthesized and accessible N,O‐bidentate auxiliary has been developed for selective C H activation under palladium catalysis. The novel auxiliary showed its first powerful application in C H functionalization of remote positions. Both C(sp²) H and C(sp³) H bonds at δ‐ and ε‐positions were effectively activated, thus giving tetrahydroquinolines, benzomorpholines, pyrrolidines, and indolines in moderate to excellent yields by palladium‐catalyzed intramolecular C H amination.     

Redox‐Triggered C?C Coupling of Diols and Alkynes: Synthesis of β,γ‐Unsaturated α‐Hydroxyketones and Furans by Ruthenium‐Catalyzed Hydrohydroxyalkylation

Direct ruthenium‐catalyzed C C coupling of alkynes and vicinal diols to form β,γ‐unsaturated ketones occurs with complete levels of regioselectivity and good to complete control over the alkene geometry. Exposure of the reaction products to substoichiometric quantities of p‐toluenesulfonic acid induces cyclodehydration to form tetrasubstituted furans. These alkyne‐diol hydrohydroxyalkylations contribute to a growing body of merged redox‐construction events that bypass the use of premetalated reagents and, hence, stoichiometric quantities of metallic by‐products.     

Palladium(0)/PAr3‐Catalyzed Intermolecular Amination of C(sp3)?H Bonds: Synthesis of β‐Amino Acids

An intermolecular C(sp³) H amination using a Pd⁰/PAr₃ catalyst was developed. The reaction begins with oxidative addition of R₂N OBz to a Pd⁰/PAr₃ catalyst and subsequent cleavage of a C(sp³) H bond by the generated Pd NR₂ intermediate. The catalytic cycle proceeds without the need for external oxidants in a similar manner to the extensively studied palladium(0)‐catalyzed C H arylation reactions. The electron‐deficient triarylphosphine ligand is crucial for this C(sp³) H amination reaction to occur.