ABSTRACT
Lithium ion selective crown ethers have been the subject of much research for a multitude of applications. Current research is aimed at structurally rigidifying crown ethers, as restructuring of the crown ether ring upon ion binding is energetically unfavorable. In this work, the lithium ion binding ability of the relatively rigid 8-crown-4 was investigated both computationally by density functional theory calculations and experimentally by 1 H and 7 Li NMR spectroscopy. Although both computational and experimental results showed 8-crown-4 to bind lithium ion, this binding was found to be weak compared to larger crown ethers. The computational analysis revealed that the complexation is driven by enthalpy rather than entropy, illustrating that rigidity is only of nominal importance. To elucidate the origin of the favorable interaction of lithium ion with crown ethers, activation strain analyses and energy decomposition analyses were performed pointing to the favorable interaction being mainly electrostatic in nature. 8-crown-4 presents the smallest crown ether reported to date capable of binding lithium ion, possessing two distinct conformations from which it is able to do so.
ABSTRACT
The Lewis acid mediated reduction of ribose-, arabinose-, xylose-, and lyxose-derived methyl and phenyl ketofuranoses with triethylsilane as nucleophile was found to proceed with good to excellent stereoselectivity to provide the 1,2-cis addition products. The methyl ketoses reacted in a more stereoselective manner than their phenyl counterparts. The stereochemical outcome of the reactions parallels the relative stability of the oxocarbenium ion conformers involved, as assessed by calculating the free energy surface maps of their complete conformational space. The Lewis acid mediated reduction allows for a direct synthesis of C-glycosides with predictable stereochemistry.
ABSTRACT
Lewis acid mediated substitution reactions using [D]triethylsilane as a nucleophile at the anomeric center of the four pentofuranoses, ribose, arabinose, xylose, and lyxose, all proceed with good to excellent stereoselectivity to provide the 1,2-cis adducts. To unravel the stereoelectronic effects underlying the striking stereoselectivity in these reactions we have mapped the energy landscapes of the complete conformational space of the oxocarbenium ions of the four pentofuranoses. The potential energy surface maps provide a detailed picture of the influence of the differently oriented substituents and their mutual interactions on the stability of the oxocarbenium ions and the maps can be used to account for the observed stereoselectivities of the addition reactions.
ABSTRACT
Although it is often assumed that the stereochemistry in Ugi multicomponent reactions is determined in the final Mumm rearrangement step, experimental and computational evidence that Ugi reactions on hydroxylated pyrrolines proceed under kinetic control is reported. The stereochemistry of the reaction is established with the addition of the isocyanide to the intermediate iminium ion, whose conformation is determined by its substitution pattern.
ABSTRACT
The reactivity of a variety of mannopyranosyl uronic acid donors was assessed in a set of competition experiments, in which two (S)-tolyl mannosyl donors were made to compete for a limited amount of promoter (NIS/TfOH). These experiments revealed that the reactivity of mannuronic acid donors is significantly higher than expected based on the electron-withdrawing capacity of the C-5 carboxylic acid ester function. A 4-O-acetyl-ß-(S)-tolyl mannuronic acid donor was found to have similar reactivity as per-O-benzyl-α-(S)-tolyl mannose.
Subject(s)
Mannose/chemistry , Uronic Acids/chemistry , Glycosylation , Molecular StructureABSTRACT
With the aim to find an efficient synthetic procedure for the construction of 2,3-diamino-2,3-dideoxy-ß-D-mannuronic acids, we evaluated three mannosyl donors: (S)-phenyl 4,6-di-O-acetyl-2,3-diazido mannopyranoside, (S)-phenyl 2,3-diazido-4,6-O-benzylidene mannopyranoside, and (S)-phenyl 2,3-diazido mannopyranosyl methyl uronate. The first two mannosylating agents are rather unselective or slightly α-selective in their condensation with three different acceptors. The mannuronic acid donor on the other hand reliably provides the desired ß-mannosidic linkage. A mechanistic rationale is put forward to account for the different behavior of the three donor types. Suitably protected 2,3-diazido mannuronic acids were employed to construct the all-cis-linked tetrasaccharide repeating unit of the capsular polysaccharide of Bacillus stearothermophilus , featuring two 2,3-diacetamido-2,3-dideoxy-ß-D-mannuronic acids.
Subject(s)
Uronic Acids/chemical synthesis , Geobacillus stearothermophilus/chemistry , Mannose/chemistry , Polysaccharides/chemistry , Stereoisomerism , Uronic Acids/chemistryABSTRACT
Mannosazide methyl uronate donors equipped with a variety of anomeric leaving groups (ß- and α-S-phenyl, ß- and α-N-phenyltrifluoroacetimidates, hydroxyl, ß-sulfoxide, and (R(s))- and (S(s))-α-sulfoxides) were subjected to activating conditions, and the results were monitored by (1)H NMR. While the S-phenyl and imidate donors all gave a conformational mixture of anomeric α-triflates, the hemiacetal and ß- and α-sulfoxides produced an oxosulfonium triflate and ß- and α-sulfonium bistriflates, respectively. The ß-S-phenyl mannosazide methyl uronate performed best in both activation experiments and glycosylation studies and provided the 1,2-cis mannosidic linkage with excellent selectivity. Consequently, an α-Glc-(1â4)-ß-ManN(3)A-SPh disaccharide, constructed by the stereoselective glycosylation of a 6-O-Fmoc-protected glucoside and ß-S-phenyl mannosazide methyl uronate, was used as the repetitive donor building block in the synthesis of tri-, penta-, and heptasaccharide fragments corresponding to the Micrococcus luteus teichuronic acid.
Subject(s)
Hexuronic Acids/chemistry , Oligosaccharides/chemical synthesis , Uronic Acids/chemistry , Uronic Acids/chemical synthesis , Carbohydrate Sequence , Glycosylation , Magnetic Resonance Spectroscopy , Oligosaccharides/chemistry , StereoisomerismABSTRACT
The search for stereoselective glycosylation reactions has occupied synthetic carbohydrate chemists for decades. Traditionally, most attention has been focused on controlling the S(N)2-like substitution of anomeric leaving groups as highlighted by Lemieux's in situ anomerization protocol and by the discovery of anomeric triflates as reactive intermediates in the stereoselective formation of beta-mannosides. Recently, it has become clear that also S(N)1-like reaction pathways can lead to highly selective glycosylation reactions. This review describes some recent examples of stereoselective glycosylations in which oxacarbenium ions are believed to be at the basis of the selectivity. Special attention is paid to the stereodirecting effect of substituents on a pyranosyl ring with an emphasis on the role of the C-5 carboxylate ester in the condensations of mannuronate ester donors.
Subject(s)
Oxygen/chemistry , Pyrans/chemistry , Glycosylation , StereoisomerismABSTRACT
Activation of mannuronic acid esters leads to a conformational mixture of alpha-anomeric triflates, in which the equatorial triflate ((1)C(4) chair) is formed preferentially. This unexpected intermediate clearly opposes the anomeric effect and is mainly stabilized by the electron-withdrawing carboxylate function at C-5. Because the anomeric center carries a significant positive charge, the (1)C(4) mannopyranosyl chair approximates the favored (3)H(4) half-chair oxacarbenium ion conformation. The excellent beta-selectivity in glycosylations of mannuronates is postulated to originate from the cooperative action of the triflate counterion and the (stereo)electronic effects governing oxacarbenium ion stabilization in the transition state leading to the 1,2-cis product.
ABSTRACT
The stereodirecting effect of the glycosyl C-5 substituent has been investigated in a series of d-pyranosyl thioglycoside donors and related to their preferred positions in the intermediate (3)H(4) and (4)H(3) half-chair oxacarbenium ions. Computational studies showed that an axially positioned C-5 carboxylate ester can stabilize the (3)H(4) half-chair oxacarbenium ion conformer by donating electron density from its carbonyl function into the electron-poor oxacarbenium ion functionality. A similar stabilization can be achieved by a C-5 benzyloxymethyl group, but the magnitude of this stabilization is significantly smaller than for the C-5 carboxylate ester. As a result, the preference of the C-5 benzyloxymethyl to occupy an axial position in the half-chair oxacarbenium ions is much reduced compared to the C-5 carboxylate ester. To minimize steric interactions, a C-5 methyl group prefers to adopt an equatorial position and therefore favors the (4)H(3) half-chair oxacarbenium ion. When all pyranosyl substituents occupy their favored position in one of the two intermediate half-chair oxacarbenium ions, highly stereoselective glycosylations can be achieved as revealed by the excellent beta-selectivity of mannuronate esters and alpha-selectivity of 6-deoxygulosides.
Subject(s)
Pyrans/chemistry , Computer Simulation , Glycosylation , Molecular Structure , Stereoisomerism , Thermodynamics , Thioglycosides/chemistryABSTRACT
Glycosylations of mannuronate ester donors proceed highly selectively to produce the 1,2-cis-linked products. We here forward a mechanistic rationale for this counterintuitive selectivity, based on the remote stereodirecting effect of the C5-carboxylate ester, which has been demonstrated using pyranosyl uronate ester devoid of ring substituents other than the C5- carboxylate ester. It is postulated that the C5-carboxylate ester prefers to occupy an axial position in the oxacarbenium intermediate, thereby favoring the formation of the (3)H4 half-chair over the (4)H3 conformer. Nucleophilic attack on the (3)H4 half-chair intermediate occurs in a beta-fashion, providing the 1,2-cis-mannuronates with excellent stereoselectivity. The potential of the mannuronate ester donors in the formation of the beta-mannosidic linkage has been capitalized upon in the construction of a mannuronic acid alginate pentamer using a convergent orthogonal glycosylation strategy.
Subject(s)
Alginates/chemical synthesis , Carboxylic Acids/chemistry , Esters/chemistry , Hexuronic Acids/chemical synthesis , Alginates/chemistry , Carbohydrate Conformation , Carbohydrate Sequence , Carboxylic Acids/chemical synthesis , Esters/chemical synthesis , Glycosylation , Hexuronic Acids/chemistry , Molecular Sequence Data , StereoisomerismABSTRACT
The glycosylation properties of gulopyranosides have been mapped out, and it is shown that gulose has an intrinsic preference for the formation of 1,2-cis-glycosidic bonds. It is postulated that this glycosylation behaviour originates from nucleophilic attack at the oxacarbenium ion, which adopts the most favourable 3H4 conformation. Building on the stereoselectivity of gulose, a guluronic acid alginate trisaccharide was assembled for the first time by using gulopyranosyl building blocks.
Subject(s)
Alginates/chemical synthesis , Hexuronic Acids/chemistry , Alginates/chemistry , Esters/chemistry , Glucose/chemistry , Glycosylation , Stereoisomerism , Substrate SpecificityABSTRACT
The photochemical reactions of a series of triaryl vinyl halides 1X in acetic acid and in acetonitrile have been studied using product analysis as a function of the time of irradiation. The quantum efficiencies of formation of the products derived from the photogenerated vinyl cations 1(+) depend on the alpha-aryl substituent, the beta-aryl substituent, the leaving group X (= bromide or chloride), and the temperature at which the irradiations are carried out. Hammett correlation or noncorrelation of the alpha-aryl substituent effects with (excited-state) substituent constants indicates that the ions 1(+) are formed directly from the excited states of 1X by heterolytic cleavage of the carbon-halogen bond. Homolytic cleavage, yielding radicals 1(*), is a parallel process: the partitioning into ion and radical occurs in the excited state. This conclusion is corroborated by the leaving group effect and the temperature effect. By performing the photochemical reactions of 1X in the presence of HOAc and/or NaOAc as well as the labeled common halide ion (82)Br(-) or (36)Cl(-), the relative reactivities of the cations 1(+) toward these nucleophiles were determined. The selectivities follow the Reactivity-Selectivity Principle. The temperature effect data show that the reactions of the cations with the anionic nucleophiles are (de)solvation controlled and their reactions with the neutral nucleophile activation controlled.
ABSTRACT
The photochemical solvolyses of 4-tert-butylcyclohex-1-enyl(phenyl)iodonium tetrafluoroborate (1) and cyclopent-1-enyl(phenyl)iodonium tetrafluoroborate (2) in methanol yield vinylic ethers and vinylic cycloalkenyliodobenzenes and cycloalkenylbenzene, which are the trapping products of the geometrically destabilized C6-ring and C5-ring vinyl cation with the solvent and with the leaving group iodobenzene. Iodonium salt 2 also yields an allylic ether and allylic cyclopentenyliodobenzenes and cyclopentenylbenzene, which are the trapping products of the C5-ring allylic cation produced from the C5-ring vinyl cation by a hydride shift in a typical carbocationic rearrangement.
Subject(s)
Cycloparaffins/chemical synthesis , Cycloparaffins/radiation effects , Ultraviolet Rays , Vinyl Compounds/chemical synthesis , Vinyl Compounds/radiation effects , Cations/chemical synthesis , Cations/chemistry , Cations/radiation effects , Cycloparaffins/chemistry , Models, Molecular , Molecular Structure , Photochemistry , Stereoisomerism , Vinyl Compounds/chemistryABSTRACT
The photochemical reactions in methanol of the vinylic halides 1-4, halostyrenes with a methyl or a trifluoromethyl substituent at the alpha- or beta-position, have been investigated quantitatively. Next to E/Z isomerization, the reactions are formation of vinyl radicals, leading to reductive dehalogenation products, and formation of vinyl cations, leading to elimination, nucleophilic substitution, and rearrangement products. The vinyl cations are parts of tight ion pairs with halide as the counterion. The elimination products are the result of beta-proton loss from the primarily generated alpha-CH(3) and alpha-CF(3) vinyl cations, or from the alpha-CH(3) vinyl cation formed from the beta-CH(3) vinyl cation via a 1,2-phenyl shift. The beta-CF(3) vinyl cation reacts with methanol yielding nucleophilic substitution products, no migration of the phenyl ring producing the alpha-CF(3) vinyl cation occurs. The alpha-CF(3) vinyl cation, which is the most destabilized vinyl cation generated thus far, gives a 1,2-fluorine shift in competition with proton loss. The experimentally derived order of stabilization of the vinyl cations photogenerated in this study, alpha-CF(3) < beta-CF(3) < beta-CH(3) < alpha-CH(3), is corroborated by quantum chemical calculations, provided the effect of solvent is taken into account.
ABSTRACT
In this paper, a rapid route toward functionalized bicyclic alkaloids is presented. In only three steps, an easily accessible carbohydrate derivative was converted into iodomethyl indolizidine 13, which can equilibrate to the corresponding iodoquinolizidine 15. We provide strong evidence that this equilibration proceeds via an aziridinium ion intermediate. Furthermore, nucleophilic substitution of the iodomethyl indolizidine as well as the aziridinium intermediate gives access to highly functionalized indolizidine and quinolizidine alkaloids.
Subject(s)
Alkaloids/chemical synthesis , Indolizines/chemical synthesis , Quinolizines/chemical synthesis , Alkylation , Aziridines/chemistry , Hydroxylation , Magnetic Resonance Spectroscopy , Molecular Conformation , StereoisomerismABSTRACT
The photochemistry of (E)-bromostyrene was investigated to determine the nature of the product-forming intermediates and to clarify the mechanism of formation of vinylic cations and vinylic radicals. Both a cation- and a radical-derived product are formed, and the ionic origin of the former product is demonstrated by significant scrambling of the label, starting from specifically deuterated (E)-bromostyrene. MO calculations show that the isolated incipient primary vinyl cation is not a metastable species, but that specific interaction with a counterion in combination with a polar environment makes it metastable. The effects of variation of the wavelength of irradiation, solvent polarity, temperature, and isotopic substitution all agree with a mechanism of direct heterolytic C-Br bond cleavage producing an ion pair followed by formation of a radical pair via electron transfer. The vinylic cation is proposed to stem directly from the indirectly populated lowest excited singlet state of bromostyrene with an energy of activation of 6.7 kcal/mol. Branching between proton loss and electron transfer in the resulting ion pair determines the ratio of cation- to radical-derived product. The E/Z-isomerization occurs in a separate process and does not involve C-Br bond cleavage.
ABSTRACT
Fluoro substitution of benzo[a]pyrene (BP) has been very useful in determining the mechanism of cytochrome P450-catalyzed oxygen transfer in the formation of 6-hydroxyBP (6-OHBP) and its resulting BP 1,6-, 3,6-, and 6,12-diones. We report here the metabolism of 1-FBP and 3-FBP, and PM3 calculations of charge densities and bond orders in the neutral molecules and radical cations of BP, 1-FBP, 3-FBP, and 6-FBP, to determine the mechanism of oxygen transfer for the formation of BP metabolites. 1-FBP and 3-FBP were metabolized by rat liver microsomes. The products were analyzed by HPLC and identified by NMR. Formation of BP 1,6-dione and BP 3,6-dione from 1-FBP and 3-FBP, respectively, can only occur by removal of the fluoro ion from C-1 and C-3, respectively, via one-electron oxidation of the substrate. The combined metabolic and theoretical studies reveal the mechanism of oxygen transfer in the P450-catalyzed formation of BP metabolites. Initial abstraction of a pi electron from BP by the [Fe(4+)=O](+)(*) of cytochrome P450 affords BP(+)(*). This is followed by oxygen transfer to the most electropositive carbon atoms, C-6, C-1, and C-3, with formation of 6-OHBP (and its quinones), 1-OHBP, and 3-OHBP, respectively, or the most electropositive 4,5-, 7,8-, and 9,10- double bonds, with formation of BP 4,5-, 7,8-, or 9,10-oxide.
Subject(s)
Benzopyrenes/metabolism , Cytochrome P-450 Enzyme System/metabolism , Microsomes, Liver/metabolism , Oxygen/metabolism , Animals , Chromatography, High Pressure Liquid , Magnetic Resonance Spectroscopy , Male , Microsomes, Liver/enzymology , Molecular Structure , Oxidation-Reduction , Rats , Rats, Wistar , Structure-Activity RelationshipABSTRACT
The photochemistry of (E)-styryl(phenyl)iodonium tetrafluoroborate in methanol and 2,2,2-trifluoroethanol as well as in dichloromethane and toluene has been investigated. In all solvents the vinylic C [bond] I bond is more photoreactive than the aromatic C [bond] I bond. Homolysis as well as heterolysis of both bonds occurs, but the latter type of cleavage predominates. In alcoholic solvents, the incipient phenyl cation produces a nucleophilic substitution product. The primary styryl cation gives nucleophilic substitution, elimination, and rearrangement products. The dependence of the photoreaction on the nucleophilicity of the solvent indicates that in the presence of good nucleophiles a 10-I-3 compound is the reactive iodonium species. In this case the reaction proceeds via an S(N)i mechanism. In the absence of good nucleophiles an 8-I-2 species gives photoreaction via an S(N)1 mechanism. This is corroborated by the solvent dependence of the UV spectra, and the product composition upon photoreaction with bromide in varying concentration. Photoreaction of the iodonium salt in a chlorinated alkane yields (E)- and (Z)-beta-fluorostyrene in a Schiemann-type reaction. Reaction in toluene yields Friedel-Crafts products. The results of the photochemical reactions are compared to those of the thermal ones, and the implications of the differences are discussed.
ABSTRACT
The dehydrohalogenation reactions of PhCH(2)-CH(2)Cl and PhCHCl-CX(2)LG (X = H, F; LG = F, Cl) with methoxide have been studied using PM3 quantum chemical calculations in vacuo and within a dielectric medium. For PhCH(2)-CH(2)Cl and PhCHCl-CH(2)Cl the loss of HCl is predicted to occur via an E2 mechanism, while for the other three compounds loss of hydrogen halide occurs via a two-step mechanism, with a hydrogen-bonded carbanion as an intermediate. The mechanistic implications of these calculations are discussed in comparison with experimental data.
