An easy access to functionalized allyl dithiocarbamates from Baylis-Hillman adducts in water

A facile and direct highly stereoselective synthesis of [E]- and [Z]-allyl dithiocarbamates has been accomplished from acetates of Baylis-Hillman (BH) adducts in catalyst-free one-pot three-component coupling reactions of carbon disulfide and amine in water under a mild and green procedure with high yields. The reaction pathway involves the nucleophilic displacement (SN2′) of BH acetates by dithiocarbamate anions. The utility of these allyl dithiocarbamates has also been demonstrated in heterocyclic chemistry. © 2009 Elsevier Science. All rights reserved     

An expedient, regioselective synthesis of 2-alkylamino- and 2-alkylthiothiazolo[5,4-e]indoles

1-Benzenesulfonyl-5-aminoindole 5, prepared from 5-nitroindole 3, was condensed with alkyl isothiocyanates and separately with carbon disulfide and alkyl bromides/iodides to furnish efficiently the corresponding N-alkyl-thioureidoindoles 6a-c and the alkyl N-(indol-5′-yl)dithiocarbamates 9a-e, respectively. Their cyclisation using N-bromosuccinimide (NBS) and 1,8-diazabicyclo[5.4.0]undec-7-ene (DBU), in the cold, followed by indolic N-deprotection, furnished regioselectively the 2-alkylamino- and the 2-alkylthiothiazolo[5,4-e]indoles 8a-c and 11a-e, respectively, in good overall yields.     

NMR studies of mixed-ligand iron(III) dithiocarbamates

¹H NMR studies of mixed-ligand iron (III) dithiocarbamates have been carried out using the following ligands: N,N-diethyldithiocarbamate, morpholinyl-N-, and piperidyl-N-carbodithioate. The ligand exchange equilibria gave all species of the general formula Fe(dtc)_n(dtc′)_3?n, where n = 0-3 with nearly random statistical distribution of Fe(Et₂dtc)_n(morphdtc)_3?n complexes. Magnetic moments of the mixed-ligand complexes have been determined. Both the magnetic moment and isotropic shift temperature dependences confirmed the cross-over properties of these mixed-ligand complexes.     

Dithiocarbamates as universal reversible addition‐fragmentation chain transfer agents

Control of the radical polymerization of acrylates, styrene and vinyl acetate has been achieved by using novel dithiocarbamates as reversible addition‐fragmentation chain transfer agents. The key parameter for the control with N,N‐disubstituted (A) or cyclic (B) dithiocarbamates was found to be the conjugation of the lone pair of electrons of the nitrogen atom with carbonyl or aromatic groups.     

SYNTHESIS OF DITHIOCARBAMATES AND SELENOTHIOCARBAMATES

Several dithiocarbamates and selenothiocarbamates were synthesized by the reaction of N N -dimethylthiocarbamoyl chloride with the corresponding thiolates and selenolates.     

Synthesis, characterization, antibacterial and cytotoxic activity of new palladium(II) complexes with dithiocarbamate ligands: X-ray structure of bis(dibenzyl-1-S:S′-dithiocarbamato)Pd(II)

Six palladium(II) dithiocarbamates of general formula Pd(AmDTC)₂, where HAmDTC = aminedithiocarbamic acid, [Pd(II) piperidinedithiocarbamate (1), Pd(II) 4-methylpiperidinedithiocarbamate (2), Pd(II) N-methylbenzyldithiocarbamate (3), Pd(II) dibenzyldithiocarbamate (4), Pd(II) dicyclohexyldithiocarbamate (5), Pd(II) N-cyclohexyl-N-methyldithiocarbamate (6)] have been synthesized and characterized by elemental analyses, FT-IR, ¹H and ¹³C NMR. The X-ray structure of Pd(II), compounds 3 and 4, showed that the ligands are chelated by both sulfur atoms with bond angles S1-Pd-S4 = 179.24(2)° and S2-Pd-S3 = 179.09(5)°, with a distorted square planar geometry around Pd. All these complexes were screened for cytotoxic and antibacterial effects and showed significant antibacterial activity and no substantial in vitro cytotoxicity indicating specificity of the compounds.     

Acylation of dithiocarbamates derived from l-ephedrine and d-pseudoephedrine

The acylation of dithiocarbamates derived from l-ephedrine and d-pseudoephedrine gives, depending on the structure of the acylating agent, acyl derivatives of the dithiocarbamates or their cyclic decomposition products, viz. oxazolidinethiones.     

An electron donor–acceptor photoactivation strategy for the synthesis of S-aryl dithiocarbamates using thianthrenium salts under mild aqueous micellar conditions

An eco-friendly and convenient method is developed herein for the synthesis of S-aryl dithiocarbamates via visible-light-induced SET process of an EDA complex between thianthrenium salt functionalized arenes and dithiocarbamate anions under mild aqueous micellar conditions. This strategy indirectly realizes the method for constructing S-aryl dithiocarbamates through site-selective C−H functionalization of arenes. Most importantly, the reaction proceeded smoothly without addition of any photocatalyst, and the by-product thianthrene is recycled in quantity, ultimately minimizing the production of chemical waste. This protocol provides a promising synthesis candidate for the construction of valuable S-aryl dithiocarbamates, which also opens up a new avenue for micellar photocatalysis.     

Dithiocarbamate mediated controlled/living free radical polymerization of methyl acrylate under 60Co γ‐ray irradiation: Conjugation effect of N‐group

The free radical polymerizations of methyl acrylate have been studied under γ‐ray irradiation in the presence of the dithiocarbamates with different N‐groups. The results indicate that the conjugation structure of the N‐group of dithiocarbamate plays an important role in living free radical polymerization. The polymerizations reveal good living characteristics in the presence of dithiocarbamates (benzyl 1H‐imidazole‐1‐carbodithioate, benzyl 1H‐pyrrole‐1‐carbodithioate, benzyl 1H‐indole‐1‐carbodithioate, and benzyl 9H‐carbazole‐9‐carbodithioate) with N‐aryl group. In contrast, the polymerization with benzyl N,N‐diethyldithiocarbamate cannot be controlled, and the obtained polymer has a broad molecular weight distribution or even crosslink occurs. Moreover, polymerization rate is influenced by the conjugation structure of the N‐group of dithiocarbamate, and the aromatic polycyclic structure of the N‐group leads to slow polymerization. © 2004 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 42: 5670–5677, 2004     

The addition reaction of acrylonitrile and methylacrylate toN-(5R-1,3,4-thiadiazol-2-yl)dithiocarbamates

A new type of dithiocarbamic acid derivatives,S-(2-X-ethyI) ethers ofN-(5R-1,3,4-thiadiazol-2-yl)-dithiocarbamic acids (X = CN, COOMe), has been synthesized by the reaction of sodiumN-(1,3,4-thiadiazol-2-yl) dithiocarbamates with acrylonitrile and methylacrylate.Deceased.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 4, pp. 749–750, April, 1994.     

A novel isocyanide-based three-component reaction: a facile synthesis of substituted 2H-pyran-3,4-dicarboxylates

An efficient method for synthesis of 2H-pyran-3,4-dicarboxylates using the three-component reaction of dithiocarbamates, dialkyl acetylenedicarboxylates, and isocyanides in solvent-free conditions is described. In these reactions, synthesis of dithiocarbamates is possibly based on the one-pot reaction of secondary amines, CS₂, and alkyl halides in solvent-free conditions without using a catalyst. The mild reaction conditions and high yields of the reaction exhibit the good synthetic advantage of these methods.     

Co(III) N,N′-diarylformamidine dithiocarbamate complexes: Synthesis,characterization, crystal structures and biological studies

Three symmetric N,N-diarylformamidine dithiocarbamates, N,N′-bis(2,6-dimethylphenyl)formamidine dithiocarbamate (DTL1), N,N′-bis(2,6-disopropylphenyl)formamidine dithiocarbamate (DTL2) and N,N′-dimesitylformamidine dithiocarbamate (DTL3), and three unsymmetric ones, N′-(2,6-dichlorophenyl-N-(2,6-dimethylphenyl)formamidine dithiocarbamate (DTL4), N′-(2,6-dichlorophenyl)-N-(2,6-diisopropylphenyl)formamidine dithiocarbamate (DTL5) and N′-(2,6-dichlorophenyl)-N-mesitylformamidine dithiocarbamate (DLT6), were reacted with chloridocobalt(III) in water to give Co-(DTL1)₃ ( 1 ), Co-(DTL2)₃ ( 2 ), Co-(DTL3)₃ ( 3 ), Co-(DTL4)₃ ( 4 ), Co-(DTL5)₃ ( 5 ) and Co-(DTL6)₃ ( 6 ). All the dithiocarbamates and complexes were characterized using ¹H NMR, ¹³C NMR, Fourier transform infrared, UV–visible and mass spectra and the purity confirmed by elemental analysis. In addition, crystal structures of complexes 1 , 2 , 4 and 5 were determined, confirming the formation of mononuclear species in which the Co(III) centers coordinated to six sulfur atoms from three dithiocarbamate ligands resulting in distorted octahedral geometries. All complexes showed moderate to good antibacterial activities against Gram-negative bacteria Escherichia coli, Salmonella typhimurium, Klebsiella pneumoniae and Pseudomonas aeruginosa even at low concentrations. None of the six were active against Gram-positive bacterium methicillin-resistant Staphylococcus aureus and only active against S. aureus at high concentrations. Complexes 5 and 6 were found to be more active than ciprofloxacin against S. typhimurium, E. coli, P. aeruginosa and K. pneumoniae and complexes with chloro-substituted ligands generally had enhanced activities. Antioxidant activities of the dithiocarbamate salts and their Co(III) complexes were also investigated using DPPH assay and the complexes were found to be more efficient. Complex 2 with an IC₅₀ value of 2.84 × 10⁻⁴ mM displayed the highest activity of all compounds tested, even outdoing ascorbic acid. The radical scavenging ability of the complexes followed the order 2 > 1 > ascorbic acid > 3 > 4 > 6 > 5 .     

Tetrahydro-2-thioxo-2H-1,3,5-thiadiazin-4-ones and their derivatives representing a novel heterocyclic ring system

The cyclization reaction between N-substituted dithiocarbamates ( 1 ) and N-substituted N-chloromethylcarbamoyl chlorides ( 2 ) gives 3,5-disubstituted tetrahydro-2-thioxo-2H-1,3,5-thiadiazin-4-ones ( 3 ). In order to decide among the theoretically possible structures 3-5 , the compounds 6a,b , containing a thioxo group instead of an oxo group as in 3a,b , as well as the S-oxide derivative of 3a was also established by X-ray structure determination.     

Selective synthesis of 2-aminobenzoxazoles and 2-mercaptobenzoxazoles by using o-aminophenols as starting material

2-Aminobenzoxazoles and 2-mercaptobenzoxazoles were selectively synthesized by treating o-aminophenols with dithiocarbamates and tetramethylthiuram disulfide (TMTD), respectively. With the promotion of NaH/CuI, the reaction of o-aminophenols with dithiocarbamates gave 2-aminobenzoxazoles with good yield (70–92%) in one pot manner, and 2-mercaptobenzoxazoles were synthesized (yield: 55–80%) in the presence of K₂CO₃ by treating o-aminophenols with tetramethylthiuram disulfide (TMTD). The feature of this method includes good to excellent yield, easy performance and broad substrate scope, which makes the protocol practical and attractive in the preparation of some potential pharmaceutically active compounds.     

Bridge cleavage reactions of cyclopalladated nitrosamines with thioamides and related compounds

The palladacycle [Pd(μ-O₂CMe){κ²C,N-4-MeC₆H₃N(Me)NO}]₂ readily undergoes bridge cleavage reactions with a variety of compounds containing donor functionalities including thioamides, 8-hydroxyquinoline, thioureas, selenoureas, acetylacetone derivatives, dithiocarbamates, xanthates, as well as bidentate N-donors to afford either the monomeric, neutral Pd(II) complexes [Pd{κ²C,N-4-MeC₆H₃N(Me)NO}{L-L}] or the monocationic complexes [Pd{κ²C,N-4-MeC₆H₃N(Me)NO}(N-N)]PF₆ in high yields. A series of 15 different complexes was prepared and fully characterised spectroscopically and, in some cases, by X-ray diffraction. It was also found that the dithiocarbamato complex undergoes a disproportionation reaction in solution to give the bis(cyclometallated) complex [Pd{κ²C,N-4-MeC₆H₃N(Me)NO}₂] as well as the bis(dithiocarbamato) complex [Pd{κ²S-S₂CNEt₂}₂].     

Copper(I) catalysis: Synthesis of N,N′-diarylated and N-aryl,N′-formylated chiral C2-symmetric diamines

Chiral N,N′-diaryl C₂-symmetric diamines and N-aryl,N′-formyl-trans-(1R,2R)-diaminocyclohexane are readily accessed by copper catalyzed N,N′-diarylation and N-aryl,N′-formylation of trans-(1R,2R)-diaminocyclohexane with aryl bromides. N,N′-diarylation using (R)-1,1′-binaphthyl-2,2′-diamine and iodobenzene gave the corresponding (R)-N,N′-diphenyl-1,1′-binaphthyl-2,2′-diamine derivative in 83% yield.     

Synthesis of dithiocarbamine derivatives on the matrix of cytisine,anabasine and d-pseudoephedrine alkaloids. Crystalline structure of N-cytisine dithiocarbamate ammonium salt

On the matrix of physiologically active alkaloids such as cytisine, anabasine, and d-pseudoephedrine the simplest alkaloid dithiocarbamates ammonium salts were synthesized by reaction with carbon disulfide in solution of ammonia in alcohol. Spatial structure of ammonium N-cytisine dithiocarbamate crystal hydrate was proved with X-ray diffraction analysis.     

A new efficient synthesis of isothiocyanates from amines using di-tert-butyl dicarbonate

Alkyl and aryl amines are converted smoothly to the corresponding isothiocyanates via the dithiocarbamates in good to excellent yields using di-tert-butyl dicarbonate (Boc₂O) and 1-3 mol % of DMAP or DABCO as catalyst. As most of the byproducts are volatile, the work-up involves simple evaporation of the reaction mixture.     

Synthesis,Structure, and Fungicidal Activity of Organotin Dithiocarbamates Derived from Pyridinamines and Aryl Diamines

A reaction of N‐benzylpyridinamines with n‐BuLi, followed by a reaction with CS₂ and R₃SnCl or R₂SnCl₂ (R = n‐Bu, PhCH₂, or Ph) gave a series of mononuclear organotin dithiocarbamates. A similar reaction of N,N'‐bis(benzyl)‐1,3‐benzenediamine and N,N'‐bis(benzyl)‐2,6‐pyridinediamine afforded dinuclear and macrocyclic organotin dithiocarbamates. All of these complexes were characterized by elemental analysis, IR, and multinuclear NMR (¹H, ¹³C, and ¹¹⁹Sn). Their structures have been confirmed by the X‐ray single crystal diffraction analysis, suggesting the dithiocarbamate groups acted as anisobidentate chelating ligands in these complexes. The primary fungicidal activity of these complexes was tested in vitro, showing that most complexes displayed good antifungal activity to Sclerotinia sclerotiorum.