Catalytic Asymmetric Three‐component Hydroacyloxylation/ 1,4‐Conjugate Addition of Ynamides

A highly enantioselective three‐component hydroacyloxylation/1,4‐conjugate addition of ortho‐hydroxybenzyl alcohols, ynamides and carboxylic acids was developed under mild reaction conditions in the presence of a chiral N,N′‐dioxide/Sc(OTf)₃ complex, which went through in situ generated ortho‐quinone methides with α‐acyloxyenamides, delivering a range of corresponding chiral α‐acyloxyenamides derivatives containing gem(1,1)‐diaryl skeletons in moderate to good yields with excellent ee values. The scale‐up experiment and further derivation showed the practicality of this catalytic system. In addition, a possible catalytic cycle and transition state model was proposed to elucidate the origin of the stereoselectivity based on X‐ray crystal structure of the α‐acyloxyenamide intermediate and product.     

The ortho‐Substituent Effect on the Ag‐Catalysed Decarboxylation of Benzoic Acids

A combined experimental and computational investigation on the Ag‐catalysed decarboxylation of benzoic acids is reported herein. The present study demonstrates that a substituent at the ortho position exerts dual effects in the decarboxylation event. On one hand, ortho‐substituted benzoic acids are inherently destabilised starting materials compared to their meta‐ and para‐substituted counterparts. On the other hand, the presence of an ortho‐electron‐withdrawing group results in an additional stabilisation of the transition state. The combination of both effects results in an overall reduction of the activation energy barrier associated with the decarboxylation event. Furthermore, the Fujita–Nishioka linear free energy relationship model indicates that steric bulk of the substituent can also exert a negative effect by destabilising the transition state of decarboxylation.     

Application of Organolithium and Related Reagents in Synthesis,Part 29 [1]. A Concise Regiospecific Conversion of Benzoic Acids into 5-(2-Carboxyphenyl)-5-phenylpent-2-enoic Acids

Summary. A convenient two-step protocol preparation of ortho-alkylated (substituent with the carbomethoxy group at the end of five carbon atoms alkyl chain) aromatic carboxylic acids from benzoic acids anilides is described. Ortho-lithiation of benzanilides and subsequent reaction of the generated bis(N- and C-ortho-)-lithiated anilides with aromatic aldehydes provided 3-arylphthalides. In the next step, these phthalides were converted into 5-(2-carboxyphenyl)-5-phenylpent-2-enoic acids by treatment with 1-methoxy-1-trimethylsilyloxybuta-1,3-diene.     

Application of Organolithium and Related Reagents in Synthesis, Part 29 [1]. A Concise Regiospecific Conversion of Benzoic Acids into 5-(2-Carboxyphenyl)-5-phenylpent-2-enoic Acids

A convenient two-step protocol preparation of ortho-alkylated (substituent with the carbomethoxy group at the end of five carbon atoms alkyl chain) aromatic carboxylic acids from benzoic acids anilides is described. Ortho-lithiation of benzanilides and subsequent reaction of the generated bis(N- and C-ortho-)-lithiated anilides with aromatic aldehydes provided 3-arylphthalides. In the next step, these phthalides were converted into 5-(2-carboxyphenyl)-5-phenylpent-2-enoic acids by treatment with 1-methoxy-1-trimethylsilyloxybuta-1,3-diene.     

A correlation of substituent effects with proton chemical shifts in aromatic tetrazolic acids

The effect of substituents on the proton chemical shifts and spin–spin coupling constants in ortho-, meta- and para-substituted 5-phenyltetrazoles (tetrazolic acids) in DMSO–CH₃CN (1:1, v/v) was studied. With the meta- and para- substituted compounds the additivity rule of chemical shifts was obeyed, thereby enabling increments characterizing the effects of individual substituents in monosubstituted benzenes to be determined. By employing the Smith and Proulx equation, the chemical shifts of the aromatic protons were correlated with the F, R and Q substituent constants. The values of these constants are 1.02, ?0.004 and 5.49, respectively, for the tetrazolyl substituent.     

Brønsted Acid Catalyzed,Conjugate Addition of β‐Dicarbonyls to In Situ Generated ortho‐Quinone Methides—Enantioselective Synthesis of 4‐Aryl‐4H‐Chromenes

We describe herein a catalytic, enantioselective process for the synthesis of 4H‐chromenes which are important structural elements of many natural products and biologically active compounds. A sequence comprising a conjugate addition of β‐diketones to in situ generated ortho‐quinone methides followed by a cyclodehydration reaction furnished 4‐aryl‐4H‐chromenes in generally excellent yields and high optical purity. A BINOL‐based chiral phosphoric acid was employed as a Brønsted acid catalyst which converted ortho‐hydroxy benzhydryl alcohols into hydrogen‐bonded ortho‐quinone methides and effected the carbon–carbon bond‐forming event with high enantioselectivity.     

Convenient use of ortho-formylphenyl thioglycoside for regioselective conjugation with glycosyl acceptors towards regioselective 1,2-cis-glycosylation

A facile methodology is proposed for regioselective conjugation between glycosyl donors and acceptors towards the development of regioselective 1,2-cis-glycosylation method. ortho-Formylphenyl 1-thio-β-d-galactopyranoside was regioselectively tethered to methyl α-d-glucopyranoside under acidic condition to furnish an 4,6-O-arylidene acetal-linked conjugate. This conjugate can be readily converted to an ether-linked 4-O- or 6-O-derivative by regioselective cleavage of the acetal ring. In the glycosylation reaction, the ether-linked 4-OH conjugate was found to show excellent 1,2-cis selectivity via an intramolecular 1,9-transfer.     

Palladium‐Catalyzed ortho‐Selective C?H Deuteration of Arenes: Evidence for Superior Reactivity of Weakly Coordinated Palladacycles

We disclose a protocol for the palladium‐catalyzed ortho‐selective C H deuteration of arenes. Phenylacetic acids and benzoic acids are suitable substrates for this reaction. This reaction offers a catalytic route to ortho‐deuterated phenylacetic acids and benzoic acids and demonstrates the sharp difference in reactivity of palladacycle intermediates held together by weak and strong coordination.     

Palladium‐Catalyzed ortho‐Selective CH Deuteration of Arenes: Evidence for Superior Reactivity of Weakly Coordinated Palladacycles

We disclose a protocol for the palladium‐catalyzed ortho‐selective C? H deuteration of arenes. Phenylacetic acids and benzoic acids are suitable substrates for this reaction. This reaction offers a catalytic route to ortho‐deuterated phenylacetic acids and benzoic acids and demonstrates the sharp difference in reactivity of palladacycle intermediates held together by weak and strong coordination.     

Simulation of13C NMR chemical shifts for polychlorinated and polybrominated oxybenzenes with two-particle increment scheme

A two-particle system of OY-Cl and OY-Br mixed increments for predicting¹³C NMR chemical shifts of polyhalogenated polyoxybenzenes has been developed. It has been found that only theortho- and para-interactions of the OY and Hal substituents contribute significantly to the¹³C chemical shifts and that theortho-effects of the OY located between Ha1 and H and those of the OY located between two Ha1 atoms are different. Additional effects are due to solvating solvents. The increment scheme is predictive over the whole class of compounds under consideration and may be realized on personal computers.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 4, pp. 617–624, April, 1994.     

Formation of Cyclic ‘ortho’-Anhydrides of Heptalene-1,2-dicarboxylic Acids

1-(Alkoixycarbonyl)heptalene-2-carboxylic acids as well as 2-(alkoxycarbonyl)heptalene-1-carboxylic acids react with the iminium salt formed from N,N-dimethylformamide (DMF) and oxalyl chloride, in the presence of an alcohol, to yield the corresponding cyclic ‘ortho’ -anhydrides (ψ-esters; cf. Schemes 2,3,6, and 8). When the alkoxy moiety of the acids and the alcohols is different, then diastereoisomeric ‘ortho’ -anhydrides are formed due to the non-planarity of the heptalene skeleton. The approach of the alcohol from the β-side is strongly favored (cf. Scheme 5 and Table 1). This effect can be attributed to the bent topology of the heptalene skeleton which sterically hinders the approach of the nucleophile from the α-side of the postulated intermediates, i.e. the charged O-alkylated anhydrides of type 19 (cf. Scheme 6). Whereas the ‘ortho’-anhydrides with four substituents in the ‘peri’ -positions of the heptalene skeleton are configurationally stable up to 100°, the ‘ortho’ -anhydrides with only three ‘peri’ -substituents slowly epimerize at 100° (cf. Scheme 7) due to the thermally induced inversion of the configuration of the heptalene skeleton.     

Efficient Synthesis of Sterically Hindered Arenes Bearing Acyclic Secondary Alkyl Groups by Suzuki–Miyaura Cross‐Couplings

Bulky P,P?O ligands were designed to inhibit isomerization and reduction side reactions during the cross coupling between sterically hindered aryl halides and alkylboronic acids. Suzuki–Miyaura cross‐couplings between di‐ortho‐substituted aryl bromides and acyclic secondary alkylboronic acids have been achieved with high yields. The method has also enabled the preparation of ortho‐alkoxy di‐ortho‐substituted arenes bearing isopropyl groups in excellent yields. The utility of the synthetic method has been demonstrated in a late‐stage modification of estrone and in the application to a new synthetic route toward gossypol.     

Synthesis of Mixed Bisamides of Cyclic ortho-Dicarboxylic Acids

A procedure was developed for preparation of bisamides of cyclic ortho-dicarboxylic acids byacylation of m- or p-phenylenediamine in acetone solution at room temperature simultaneously with twodifferent anhydrides of cyclic or aromatic ortho-dicarboxylic acids; another process consisted in treating ananhydride of aromatic or cyclic dicarboxylic acid with monoamide of cis-4-cyclohexene-1'2-dicarboxylicacid in dimethylformamide at room temperature.     

Facile Synthesis of Alkylidene Phthalides by Rhodium-Catalyzed Domino C−H Acylation/Annulation of Benzamides with Aliphatic Carboxylic Acids

The Rh-catalyzed ortho-C(sp²)−H functionalization of 8-aminoquinoline-derived benzamides with aliphatic acyl fluorides generated in situ from the corresponding acids has been developed. This reaction initiated with 8-aminoquinoline-directed ortho-C(sp²)−H acylation, which was accompanied by subsequent intramolecular nucleophilic acyl substitution of amide group to produce alkylidene phthalides This approach exhibits high stereo-selectivity for Z-isomer products, and tolerates a variety of functional groups as well as aliphatic carboxylic acids with diverse structural scaffolds.     

Synergistic Rhodium/Phosphoric Acid Catalysis for the Enantioselective Addition of Oxonium Ylides to ortho‐Quinone Methides

We report herein a powerful and highly stereoselective protocol for the domino‐type reaction of diazoesters with ortho‐quinone methides generated in situ to furnish densely functionalized chromans with three contiguous stereogenic centers. A transition‐metal and a Brønsted acid catalyst were shown to act synergistically to produce a transient oxonium ylide and ortho‐quinone methide, respectively, in two distinct cycles. These intermediates underwent subsequent coupling in a conjugate‐addition–hemiacetalization event in generally good yield with excellent diastereo‐ and enantioselectivity.     

Die Protonierung von 1-Formyl- und 1-Acetyl-azulenen

NMR. data show that protonation of 1-formyl-azulene yields essentially a one-to-one mixture of conjugate acids in which the hydroxyl group assumes the syn-planar or anti-planar configuration relative to the tropylium nucleus. The presence of a minute amount of protonation in position 3 is demonstrated by the rapid hydrogendeuterium exchange in this position. Steric interference in 1-formyl-azulenes with a methyl group in the peri position 8 favours the anti-planar configuration. As shown by one example, the conjugate acids of 1-acetyl-azulenes without substituents in positions 2 or 8 assume the anti-planar configuration. In 1-acetyl-azulenes carrying a methyl group in position 8, addition of a proton to the carbon centre 1 is the preferred route of protonation, as a consequence of the accompanying strain release.     

Determination of amino acids in human blood serum by reversed-phase high-performance liquid chromatography in the isocratic elution mode

A procedure is developed for the determination of 15 amino acids in human blood serum usingortho-phthalic aldehyde in combination with 2-mercaptoethanol or sodium sulfite as the reagent for the precolumn synthesis of derivatives with their subsequent separation by reversed-phase high-performance liquid chromatography in the isocratic elution mode using electrochemical detection. Conditions of the quantitative conversion of amino acids to corresponding derivatives were determined;ortho-phthalic—mercaptoethanol andortho-phthalic/sulfite derivatives of amino acids are stable during the whole cycle of analysis. The total time of separation is 80 min. The detection limits are 0.5-5 pmol (at the signal-to-noise ratio equal to 2). The procedure is used for the determination of glutamic acid, asparagine, serine, glutamine, histidine, taurine, alanine, arginine, methionine, isoleucine, ornithine, leucine, phenylalanine, lysine, and tryptophane in blood serum of healthy donors and of sick with alcoholism before and after treatment     

Microwave‐Promoted Pd‐Catalyzed Synthesis of Dibenzofurans from Ortho‐Arylphenols

ortho‐Aryl phenols, synthesized via protecting group free Suzuki–Miyaura coupling of ortho‐halophenols and arene boronic acids, undergo a cyclization to dibenzofurans via oxidative C–H activation. The reaction proceeds under microwave irradiation in short reaction times using catalytic amounts of Pd(OAc)₂ without additional ligands.     

The preparation of benzoisothiazolo[1,2‐b][1,2]isoquinolin‐11‐one‐1,1‐dioxides from dilithiated ortho‐toluic acids and lithiated methyl 2‐(aminosulfonyl)benzoate

Select dilithiated ortho‐toluic acids were prepared in excess lithium diisopropylamide and condensed with methyl 2‐(aminosulfonyl)benzoate followed by a twofold cyclization of intermediates to afford benzoisothiazolo[1,2‐b][1,2]isoquinolin‐11‐one‐1,1‐dioxides, a new fused‐ring heterocyclic system.     

Metalations utilizing aryllithiums; ortho-functionalization of p-bromoanisole (pBrA)

An ortho-metalation protocol has been developed, which permits the survival of a bromine substituent in p-bromoanisole. Eight derivatives of the generated ortho-lithiated intermediate have been prepared. A neglected metalation concept is being explored here; one which proposes that minimizing the pK_a difference between the aryl substrate and the conjugate acid of the metalating agent will lead to a regiospecific and selective metalation process.