Absolute stereochemistry of allylic alcohols,amines, and other ene moieties: a microscale cross metathesis/exciton chirality protocol

A microscale chemical/chiroptical protocol for the determination of absolute configurations of allylic alcohols, amines, and related systems has been developed. The method is based on the conversion of the double bonds into a styrene, lambdamax 248 nm (epsilon 15 000), or other styrenoid chromophores by cross olefin metathesis. The obtained styrenoid chromophore then couples with the allylic acylate to yield a distinct couplet. The proposed method allows one to determine the absolute configuration of both moieties flanking the double bond. It also overcomes the restriction of the conventional allylic benzoate method that gives rise to weak CD couplet, for which in many cases only one wing of the couplet is observable.     

Structure of polymeric coumarins. I. Determination of the double bonds in copolymers and the initial coumarins by ozonization

The paper gives the results obtained in a study of the structure of coumarin derivatives by the following metheds: ozonization of the double bonds in the monomeric and polymeric coumarins, and also in mixtures of polyvinylpyrrolidone with monomeric coumarins, and the treatment of the monomeric coumarins under the conditions of radical copolymerization but without the participation of N-vinylpyrrolidone.     

A novel sodium carbonate-catalyzed regioselective synthesis of pyrano[2,3-h]coumarins using a three-component reaction

In this work, a novel, convenient, and efficient approach to the synthesis of pyrano[2,3-h]coumarins has been reported based on the multicomponent reaction. The one-pot reaction between 5,7-dihydroxy-4-methylcoumarin, dialkyl acetylenedicarboxylate and aromatic aldehydes catalyzed by sodium carbonate lead to the formation of a novel class of pyrano[2,3-h]coumarin derivatives. High atom-economy, excellent yields, simple procedure, and mild reaction conditions are the important features of this protocol. This method allows access to a variety of pyrano[2,3-h]coumarins via using a broad substrate scope.     

5-Demethoxy-10′-ethoxyexotimarin F,a New Coumarin with MAO-B Inhibitory Potential from Murraya exotica L.

Rutaceae plants are known for being a rich source of coumarins. Preliminary molecular docking showed that there was no significant difference for coumarins in Clausena and Murraya, both of which had high scoring values and showed good potential inhibitory activity to the MAO-B enzyme. Overall, 32 coumarins were isolated from Murraya exotica L., including a new coumarin 5-demethoxy-10′-ethoxyexotimarin F (1). Their structures were elucidated on the basis of a comprehensive analysis of 1D and 2D NMR and HRMS spectroscopic data, and the absolute configurations were assigned via a comparison of the specific rotations and the ECD exciton coupling method. The potential of new coumarin (1) as a selective inhibitor of MAO-B was initially evaluated through molecular docking and pharmacophore studies. Compound (1) showed selectivity for the MAO-B isoenzyme and inhibitory activity in the sub-micromolar range with an IC₅₀ value of 153.25 ± 1.58 nM (MAO-B selectivity index > 172).     

Structure of polymeric coumarins. I. Determination of the double bonds in copolymers and the initial coumarins by ozonization

The paper gives the results obtained in a study of the structure of coumarin derivatives by the following metheds: ozonization of the double bonds in the monomeric and polymeric coumarins, and also in mixtures of polyvinylpyrrolidone with monomeric coumarins, and the treatment of the monomeric coumarins under the conditions of radical copolymerization but without the participation of N-vinylpyrrolidone.Institute of High-Molecular-Weight Compounds, Academy of Sciences of the USSR, Leningrad. Translated from Khimiya Prirodnykh Soedinenii, No. 5, pp. 637–642, September–October, 1979.     

Diversity‐Oriented Synthesis of Furo[3,2‐c]coumarins and Benzofuranyl Chromenones through Chemoselective Acylation/Wittig Reaction

A highly efficient and chemoselective one‐pot protocol for the diversity‐oriented synthesis of two types of coumarin‐based formal cross‐coupling adducts, furo[3,2‐c]coumarins and 3‐benzofuranyl chromenones, is described. Key attributes of the methodology are an initial chemoselective acylation of functionalized phosphorus zwitterions and a subsequent chemoselective intramolecular Wittig reaction that preferentially resulted in one of the two coumarin derivatives in high yield, depending on relative reactivities and the addition sequence of the acylating agents.     

Total syntheses of furaquinocin A, B, and E

A modular approach to the total synthesis of furaquinocins culminated in the total syntheses of furaquinocin A, B, and E. A Pd-catalyzed dynamic kinetic asymmetric transformation (DYKAT) on carbonates derived from Baylis-Hillman adducts, followed by a reductive Heck cyclization allows the enantio- and diastereoselective construction of dihydrobenzofuran 32. Introduction of a double unsatured side chain via Horner-Wadsworth-Emmons reaction and assembly of the naphthoquinone with squaric acid based methodology leads to furaquinocin E. The use of differentially substituted squaric acid derivatives allows the synthesis of three analogues of furaquinocin E. The additional stereocenters in furaquinocin A and B can be introduced with a diastereoselective Sakurai allylation. The stereoselective elongation of the side chain is possible using cross metathesis or ring closing metathesis. The obtained late-stage intermediates were successfully transformed to furaquinocin A and B.     

Syntheses of furo[3,4-c]coumarins and related furyl coumarin derivatives via intramolecular Wittig reactions

A new and general strategy for highly functional furo[3,4-c]coumarins and related furyl coumarin derivatives has been developed, which is based on an extraordinarily facile intramolecular Wittig reaction, starting from α,β-unsaturated ketones, tributylphosphine, and acyl chlorides. The phosphorus ylides were proposed to be the key intermediates for constructing the crucial furan ring, leading to a wide variety of substituted furyl coumarins in one step.     

A CD exciton chirality method for determination of the absolute configuration of threo-beta-aryl-beta-hydroxy-alpha-amino acid derivatives

The absolute configuration of threo-beta-aryl-beta-hydroxy-alpha-amino acids was studied by CD exciton chirality method using 7-diethylaminocoumarin-3-carboxylate as a red-shifted chromophore. Bischromophoric derivatives for a series of threo-beta-aryl-beta-hydroxy-alpha-amino acids (3a-h) were prepared and their CD spectra measured in CH2Cl2. By combining the data of CD and NMR coupling constants, we are able to correlate their preferred conformer (B) and the positive CD to the corresponding (2S,3R)-absolute configuration. These results are consistent with those obtained from serine and threonine derivatives, which represent the simplest form of beta-hydroxy-alpha-amino acids. This CD method could thus become a general method for determining the absolute configuration of threo-beta-aryl-beta-hydroxy-alpha-amino acids.     

Side‐Chain Modification and “Grafting Onto” via Olefin Cross‐Metathesis

Olefin cross‐metathesis is introduced as a versatile polymer side‐chain modification technique. The reaction of a poly(2‐oxazoline) featuring terminal double bonds in the side chains with a variety of functional acrylates has been successfully performed in the presence of Hoveyda–Grubbs second‐generation catalyst. Self‐metathesis, which would lead to polymer–polymer coupling, can be avoided by using an excess of the cross‐metathesis partner and a catalyst loading of 5 mol%. The results suggest that bulky acrylates reduce chain–chain coupling due to self‐metathesis. Moreover, different functional groups such as alkyl chains, hydroxyl, and allyl acetate groups, as well as an oligomeric poly(ethylene glycol) and a perfluorinated alkyl chain have been grafted with quantitative conversions.     

A facile synthesis of highly functionalized 4-arylcoumarins via Kostanecki reactions mediated by DBU

An efficient synthesis of 4-arylcoumarins has been accomplished via Kostanecki reactions of 2-hydroxybenzophenones with acetic anhydride employing DBU at ambient temperature. Using the same strategy, several 2-acyloxybenzophenone derivatives were readily converted to 3,4-difunctionalized coumarins. This protocol offers a notable improvement in reaction conditions for coumarin synthesis and takes advantage of its synthetic capability, especially for highly functionalized 4-arylcoumarins with structural diversity.     

As low as reasonably achievable catalyst loadings in the cross metathesis of olefins with ethyl acrylate

A series of ruthenium catalysts for olefin metathesis have been screened in the cross metathesis of 1,9-decadiene with ethyl acrylate. Under optimized reaction conditions a catalyst loading of only 100 ppm in respect to double bonds was sufficient for complete conversion of the diene.     

Synthesis of nonracemic allylic hydroxy phosphonates via alkene cross metathesis

Allylic hydroxy phosphonates and their derivatives can be interconverted by using cross metathesis with second generation Grubbs catalyst. The absolute stereochemistry of the starting phosphonate is conserved in the product. Cross metathesis reaction of the acrolein-derived phosphonate 2a yields a series of functionalized allylic hydroxy phosphonates. However, the cross metathesis reaction is often accompanied by competing dimerization and alkene migration reactions leading to a reduction in yield. The cinnamaldehyde- and crotonaldehyde-derived phosphonates 2b and 2c were also examined. In general, the metathesis reactions of phosphonates 2b and 2c are considerably slower than those for phosphonate 2a leading to mixtures. Several hydroxyl-protected derivatives of the phosphonate 2a (methyl carbonate 3a, acetate 4a, N-tosyl carbamate 5a, TBDMS 6a, and acetoacetate 7a) undergo metathesis without competing side reactions to give substituted allylic phosphonates in good to excellent yield.     

New caged coumarin fluorophores with extraordinary uncaging cross sections suitable for biological imaging applications

Photocaged fluorescent molecules are important research tools for tracking molecular dynamics with high spatiotemporal resolution in biological systems. We have designed and synthesized a new class of caged coumarin fluorophores. These coumarin cages displayed more than 200-fold fluorescence enhancement after UV photolysis. Remarkably, the uncaging cross section of a 1-(2-nitrophenyl)ethyl (NPE)-caged coumarin is 6600 at wavelength of 365 nm, about 2 orders of magnitude higher than previously described caged fluorophores. Product analysis of the photolytic reaction showed clean conversion of NPE-caged coumarin to 2-nitrosoacetophenone and the parent coumarin, suggesting that the mechanism of the photolysis follows the known photochemical reaction pathway of the 2-nitrobenzyl group. We have also measured the two-photon uncaging cross sections of NPE-caged coumarins 2a and 5 at 740 nm to be near 1 Goeppert-Mayer (GM). The mechanistic study, together with the two-photon uncaging data, suggested that the coumarin moiety serves as an antenna to enhance the light harvesting efficiency of the coumarin cage and that the photonic energy absorbed by coumarin was utilized efficiently to photolyze the NPE group. Future explorations of this type of "substrate-assisted photolysis" may yield other cages of high uncaging cross sections. For cellular imaging applications, we prepared a cell permeable and caged coumarin fluorophore, NPE-HCCC2/AM (10), which can be loaded into fully intact cells to high concentrations. Initial tests of this probe in a number of cultured mammalian cells showed desired properties for the in vivo imaging applications. The combined advantages of robust fluorescence contrast enhancement, remarkably high uncaging cross sections, noninvasive cellular delivery, and flexible chemistry for bioconjugations should generate broad applications of these caged coumarins in biochemical and biological research.     

Recent Advances in the Synthesis of Coumarin Derivatives via Knoevenagel Condensation: A Review

The synthesis of coumarins through Knoevenagel condensation is one of the most important processes in synthetic organic chemistry and medicinal chemistry. Compounds including a coumarin (2-oxo-2H-1-benzopyran) backbone have a wide range of application in the pharmaceutical field. Thus, many methodologies have been developed for the synthesis of this important class of compounds. However, some methods are always associated with toxic and corrosive catalysts, longer reaction time, poor yield, less purity, and by-products along with the desired product. Furthermore, some of these processes are not efficient and environmentally friendly. Therefore, mild, efficient, and environmentally friendly protocols have been developed recently by many scientists for the synthesis of coumarin derivatives via Knoevenagel condensation with good yield and purity. In this review, we have summarized various methods for the synthesis of coumarins via Knoevenagel condensation.     

Sequential Pd(II)-Pd(0) catalysis for the rapid synthesis of coumarins

Electrophilic palladium-catalyzed cycloisomerization of brominated aryl propiolates produces brominated coumarins. The brominated coumarins can be diversified by reduction of the Pd(II) catalyst to Pd(0) followed by Suzuki, Sonogashira, Heck, or Hartwig-Buchwald coupling. Thus, a single loading of precatalyst can be used to conduct sequential reactions, allowing the synthesis of functionalized coumarins. Extension of this methodology toward the synthesis of coumarin libraries is discussed.     

Relative and absolute configurations of ganefromycin alpha

The full structure of ganefromycin alpha has been determined. The relative configurations were determined from 3JH,H coupling constants and NOE data, while the absolute configurations in moleties A and B were determined separately by difference CD of their acylate derivatives, which showed typical exciton couplets. The configurations of the stereogenic centers in ganefromycin alpha are 8S, 9S, 11R, 12S, 13S, 21S, 22R, 23R, 24R, and 26S.     

13C NMR spectroscopy of coumarin derivatives

The ¹³C chemical shifts of 209 naturally occurring and synthetic coumarin derivatives are listed and a number of methods for signal assignments are explained. Substituent effects on ¹³C chemical shifts (SCS) in monosubstituted coumarins and non-additivities of SCS in coumarins with more than one substituent are discussed in detail.     

Enantioselective Synthesis of [b]-Annulated Azepane Scaffolds

Cyclopenta-, benzo-, and cyclohepta[b]-annulated azepane scaffolds were prepared in two steps from optically active cyclic α-allyl-β-oxoesters. The first step was ruthenium-catalyzed olefin cross metathesis with acrylonitrile. The second step was palladium-catalyzed dihydrogenation which consists of three consecutive processes: The hydrogenation of the C−C double and C−N triple bonds was followed by the reductive amination via the iminium ion formed in situ from the primary amino function and the endocyclic carbonyl group. This last step gave, stereoselectively, the annulated azepanes with relative trans-configuration. The amino function and the ester group define two points for further diversification of the scaffolds. The trifluoroacetyl derivatives allowed to establish the enantiopurity of the products to be 97–98 % ee by GLC on a chiral phase. The relative trans-configurations and in one case also the absolute (R,R)-configuration was established by X-ray crystallography.     

Synthesis of arylated chalcone derivatives via palladium cross-coupling reactions

A useful protocol for arylation of the olefin double bond of chalcones to afford tri- and tetra-substituted chalcone derivatives is reported. The protocol begins with the Heck reaction between chalcones and aryl iodides providing β-arylchalcones. This reaction tolerates various functional groups on both rings, as well as deactivated aryl iodides. The products are obtained in moderate to excellent yields and the (E)-β-arylchalcones (E:Z?>?96:4) can be isolated via precipitation. Competitive Heck reactions pointed to a significant effect of ring one substituents on the reaction rate, while substituents on ring two have a much smaller effect. To access α,β-diarylchalcones, a sequential bromination-Suzuki cross coupling strategy was applied to the β-arylated compounds which afforded double arylated chalcone derivatives in 60–99% yield over two steps.