Synthesis of unsaturated esters of pyridine-and quinolinecarboxylic acids

The vinyl esters of pyridine-2-and -4-carboxylic acids, the propargyl esters of pyridine-2-, -3-, and-4-carboxylic acids, the vinyl, allyl, and propargyl esters of quinoline-2-, -4-, and -8-carboxylic acids, and the allyl ester of 2-methylisonicotinic acid have been synthesized.     

Propargyl‐Assisted Selective Amidation Applied in C‐terminal Glycine Peptide Conjugation

Alkyl esters, such as propargyl esters, typically lack the electron‐withdrawing inductive effects needed to participate in nucleophilic acyl substitution reactions. Herein, we report an unusual observation in which glycine propargyl ester derivatives displayed selective, base‐independent reactivity towards linear alkylamines under mild, metal‐free conditions. Through global reaction route mapping (GRRM) modeling calculations, it is predicted that these observations may be governed by factors related to hydrogen‐bonding and intermolecular interactions, rather than electron‐withdrawing inductive effects. Based on this concept of propargyl‐assisted selective amidation, a direct application was made to develop a novel site‐specific C‐terminal glycine peptide bioconjugation technique as a proof‐of‐concept, which relies upon the selective reactivity of glycine propargyl esters over that of aspartate and glutamate side‐chain‐linked propargyl esters.     

Synthesis of o-Carboranyl Containing Esters of Pentavalent Phosphorus Acids

Abstract

A new method for the synthesis of o-carboranyl containing phosphoric, phosphonic and phosphinic acid esters, where the o-carboranil group is in the ester group, has been developed. The propargyl esters of these acids were prapared in two ways: by the reaction of phosphorus acid salts with propargyl chlorid and by interaction of propargyl alcohol with acid chlorides in the presence of Et₃N. The propargyl esters have been converted into carboranyl containing compounds upon treatment with decaborane and dimethyl aniline     

A hierarchy of aryloxide deprotection by boron tribromide

Aryl propargyl ethers and esters are cleaved selectively in the presence of aryl methyl ethers and esters by boron tribromide in dichloromethane. Under the same conditions, allyl ethers undergo very rapid Claisen rearrangement, and benzyl ethers are also cleaved more rapidly than propargyl. A mechanism involving intramolecular delivery of bromide to the propargyl terminus is proposed. [reaction: see text]     

Cycloaddition accompanied by sigmatropic shift of dithiocarboxylic esters with dimethyl acetylenedicarboxylate

Allyl, propargyl and benzyl dithiocarboxylic esters react with dimethyl acetylenedicarboxylate to form 1,3-dithioles, with migration of the allyl, propargyl or benzyl group.     

Synthesis of aromatic ketones by a transition metal-catalyzed tandem sequence

Both simple Ag(I) and Au(I) are effective catalysts for a tandem [3,3]-sigmatropic rearrangement/formal Myers-Saito cyclization of propargyl esters to form aromatic ketones. A mechanism in which the metal catalyzes both of these processes through alkyne activation is proposed. By using this method a wide range of aromatic structures including naphthyl, anthracenyl and indole ketones are available from readily available propargyl esters.     

Cascade synthesis of 3-quinolinecarboxylic ester via benzylation/ propargylation-cyclization

Reactions of 2-amino-aryl alcohols with beta-ketoesters catalyzed by a catalytic amount of FeCl3 via tandem benzylation-cyclization produce the corresponding 3-quinolinecarboxylic esters in good to high yields. Extending this methodology to propargylation-cyclization, 2-nitrophenyl propargyl alcohols with beta-ketoesters catalyzed by FeCl3 and SnCl2 also produce the 4-alkyne-3-quinolinecarboxylic esters. The mechanistic details of this benzylation/propargylation and cyclization cascade process are also discussed.     

Facile synthesis of unusual glycosyl carbamates and amino acid glycosides from propargyl 1,2-orthoesters as glycosyl donors

Propargyl 1,2-O-orthoesters are exploited for the synthesis of 1,2-trans O-glycosides of protected amino acids. N-Fmoc- and N-Cbz protected serine/threonine - benzyl/methyl esters reacted well with glucosyl-, galactosyl-, mannosyl- and lactosyl- derived propargyl 1,2-orthoesters affording respective 1,2-trans glycosides in good yields under AuBr(3)/4 ? MS Powder/CH(2)Cl(2)/rt. t-Boc serine derivative gave serine 1,2-orthoester and glycosyl carbamate. Optimized conditions enabled preparation of new glycosyl carbamates from N-Boc protected amines in a single step using gold catalysts and propargyl 1,2-orthoesters in excellent yields.     

A mild C-O bond formation catalyzed by a rhenium-oxo complex

A mild method for the regioselective synthesis of propargyl ethers by the coupling of propargyl alcohols with a range of other alcohols is described. The method employs an air- and moisture-tolerant rhenium-oxo complex ((dppm)ReOCl3) as a catalyst for the formation of sp3-carbon-oxygen bonds without the need for prior activation of the propargyl alcohol or deprotonation of the alcohol nucleophile. A broad range of functional groups is tolerated, including aryl halides, olefins, esters, and acid-labile functional groups such as acetals. Furthermore, displacement of the alcohol occurs preferentially even in the presence of other electrophiles such as primary alkyl halides and conjugated esters.     

Gold-catalyzed formal [3 + 3] and [4 + 2] cycloaddition reactions of nitrosobenzenes with alkenylgold carbenoids

We report two new formal cycloaddition reactions between nitrosobenzenes and alkenylgold carbenoids. We obtained quinoline oxides 3 in satisfactory yields from the gold-catalyzed [3 + 3]-cycloadditions between nitrosobenzenes and alkenyldiazo esters 1. For propargyl esters 5, its resulting gold carbenes react with nitrosobenzene to give alkenylimine 8, followed by a [4 + 2]-cycloaddition with nitrosobenzene.     

Synthesis of N-[5-alkoxy-2(5H)-furanonyl] amino acid propargyl esters

Using K₂CO₃ as a base and CH₃CN as solvent, different kinds of N-[5-alkoxy-2(5H)-furanonyl] amino acids were reacted with propargyl bromide via substitution reaction at 40?°C to give 16 N-[5-alkoxy-2(5H)-furanonyl] amino acid propargyl esters with the yields of 44?C85% (mostly over 74%). The structures of all newly synthesized compounds were elucidated and confirmed by FTIR, UV, ¹H NMR, ¹³C NMR, MS, and elemental analysis. The rapid, efficient, and brief synthesis of the series propargyl esters with multiple bioactive units, will afford not only a basis for the activity test of potential drug molecules, but also an important synthetic strategy for 2(5H)-furanone derivatives with polyfunctional groups.     

A DDQ-promoted metal-free cross-coupling of 1,3-diarylpropynes with hydroxyl via Sp C-H bond activation to form C-O bond

A metal-free coupling reaction between 1,3-diarylpropynes and alcohols/phenols/acids via propargylic sp³ C-H bonds activation and C-O bond formation reaction promoted by DDQ was realized. The reaction afforded series of propargyl ethers, propargyl esters and propargyl ketals.     

A crossed beams study of the reaction of carbon atoms, C(3Pj), with vinyl cyanide, C2H3CN(X 1A')--investigating the formation of cyano propargyl radicals

The chemical dynamics of the reaction of ground state carbon atoms, C(3Pj), with vinyl cyanide, C2H3CN(X 1A'), were examined under single collision conditions at collision energies of 29.9 and 43.9 kJ mol(-1) using the crossed molecular beams approach. The experimental studies were combined with electronic structure calculations on the triplet C4H3N potential energy surface (H. F. Su, R. I. Kaiser, A. H. H. Chang, J. Chem. Phys., 2005, 122, 074320). Our investigations suggest that the reaction follows indirect scattering dynamics via addition of the carbon atom to the carbon-carbon double bond of the vinyl cyanide molecule yielding a cyano cyclopropylidene collision complex. The latter undergoes ring opening to form cis/trans triplet cyano allene which fragments predominantly to the 1-cyano propargyl radical via tight exit transition states; the 3-cyano propargyl isomer was inferred to be formed at least a factor of two less; also, no molecular hydrogen elimination channel was observed experimentally. These results are in agreement with the computational studies predicting solely the existence of a carbon versus hydrogen atom exchange pathway and the dominance of the 1-cyano propargyl radical product. The discovery of the cyano propargyl radical in the reaction of atomic carbon with vinyl cyanide under single collision conditions implies that this molecule can be an important reaction intermediate in combustion flames and also in extraterrestrial environments (cold molecular clouds, circumstellar envelopes of carbon stars) which could lead to the formation of cyano benzene (C6H5CN) upon reaction with a propargyl radical.     

Some new dienophiles in the diels-alder reaction with active cyclic dienes

A comparative study of the Diels-Alder reaction have been carried out for three types of cyclic dienes: cyclopentadiene (CPD), hexachlorocyclopentadiene (HCP), and tetrachloro-1,2-benzoquinone (TCBQ) with dienophiles of five types: monosubstituted acetylenes (propargyl alcohol and its esters), conjugated amines (allyl acetylene, allyl ethynyldimethylcarbonol and its esters), conjugated dienes (2-methylhexadiene-3,5-ol-2 and its esters, 1-ethoxy- and 1-ethoxycarbonylbutadiene-1,3), and conjugated trienes (hexatriene-1,3,5 and 5-methylhexatriene-1,3,5).It was found that conjugated trienes react with dienes of all types under mild conditions and give only the monoadducts through the terminal vinyl or ethynyl group.     

In-MEDIATED ALLYLATION OF α-KETO ESTERS WITH ALLYL HALIDES*

The chemoselective reaction of α-keto esters with allyl halides, propargyl bromides, and allenyl bromide using indium metal afforded α-hydroxy-γ,δ-unsaturated esters in good to excellent yields under mild conditions.

     

Terminal Alkyne-Ethylene Cross-Metathesis: Reaction of 1-Substituted Propargyl Esters at Elevated Ethylene Pressure

Substituted propargylic esters, resistant to complete ethylene cross-metathesis at ambient pressure, underwent cross-metathesis with ethylene at elevated pressure (4 atm) to give 2-substituted butadienes in good to excellent yields. Enantioenriched propargylic acetates, obtained through enzymatic kinetic resolution of secondary propargyl alcohols, similarly underwent ethylene metathesis with retention of stereochemistry at the chiral center.     

Trends in structure–toxicity relationships for carbonyl-containing α,β-unsaturated compounds

Using toxicity data for 30 aliphatic polarized α,β-unsaturated derivatives of esters, aldehydes, and ketones, a series of six structure–toxicity relationships were evaluated. The structure feature of all assessed compounds, an acetylenic or olefinic moiety conjugated to a carbonyl group, is inherently electrophilic and conveys the capacity to exhibit enhanced toxicity. However, the toxic potency of α,β-unsaturated carbonyl compounds is dependent on the specific molecular structure with several trends being observed. Specific observations include: (1) between homologues, the acetylenic-substituted derivative was more toxic than the corresponding olefinic-substituted one, respectively; (2) between olefinic-homologues, terminal vinyl-substituted derivative was more toxic than the internal vinylene-substituted one; (3) within α,β-unsaturated ketones, methyl substitution on the vinyl carbon atoms reduces toxicity with methyl-substitution on the carbon atom farthest from the carbonyl group exhibiting the greater inhibition; (4) between α,β-unsaturated carbonyl compounds with the carbon–carbon double bond on the end of the molecule (vinyl ketones) and those with carbon–oxygen double bonds on the end of the molecule (aldehydes), the ketones are more toxic than the aldehydes; (5) between homologues of α,β-unsaturated esters, those with additional unsaturated moieties (allyl, propargyl, or vinyl groups) were more toxic than homologues having relevant unsaturated moieties (propyl or ethyl groups); (6) between α,β-unsaturated carbonyl compounds with different shaped alkyl-groups (i.e. different degrees of branching), homologues with straight-chain hydrocarbon moieties were more toxic than those with branched groups.     

Methylpentanediolborane: easy access to new air- and chromatography-stable, highly functionalized vinylboronates

Methylpentanediolborane (MPBH) 1 can be prepared easily by reaction of hexyleneglycol with BH3/DMS or B2H6 generated from NaBH4 and I2. MPBH hydroborates stereo- and regioselectively highly functionalized alkynes, including propargyl bromide and propionaldehyde acetal. MPBH compares favorably with pinacolborane in terms of reactivity. The obtained vinylboronic esters are air- and chromatography-stable.     

Transition Metal-Free Alkyne-Aldehyde Reductive C−C Coupling trough Cascade Borylation/Olefin Isomerization

A direct approach to γ-keto esters through cascade alkyne-aldehyde reductive C−C coupling of propargyl esters and aromatic aldehydes under transition-metal-free (TM-free) fashion was developed. Compared with multistep processes, this procedure provides a fast path using commercially available materials and could be handled conveniently to produce various γ-keto esters in moderate yields.     

Allylstannation: VII. Preparation of carboxylic acid 1-alkene-4-yl and 1-alkyne-4-yl esters by transalkoxylation of 4-n-dibutylchlorostannoxy-1-alkenes and 4-n-dibutylchlorostannoxy-1-alkynes with acyl chlorides

Carboxylic acid 1-alkene-4-yl and 1-alkyne-4-yl, esters (RCH(CH₂CHCH₂)OCOR′ ad RCH(CH₂CCH)OCOR′, R = R′ or R ≠ R′ = alkyl or alkenyl group) can be readily prepared in high yields by transalkoxylation reactions between 4-n-dibutylchlorostannoxy-1-alkenes or 4-n-dibutylchlorostannoxy-1-alkynes with acyl chlorides. This represents a general route for preparation of esters containing allyl or propargyl groups.