Synthesis of thiazole aminophosphine oxides, aminophosphonic and aminophosphinic acids and Cu(II) binding abilities of thiazole aminophosphonic acids

A series of new aminophosphine oxides, aminophosphonic and aminophosphinic acids derived from thiazole was synthesized by addition of phosphine oxides or silylated phosphorus esters to the corresponding thiazole aldimines. The thiazole aldimines were obtained from 2-thiazole aldehyde and primary amines by a standard procedure. The corresponding phosphine oxides were obtained by alkylation of diethyl phosphite or ethyl phenylphosphinate with the appropriate Grignard reagents. The silylated phosphorus esters were prepared from trimethyl phosphite and from methyl- or phenylphosphinic ethyl ester by treatment with bromotrimethylsilane. The coordination ability towards Cu(II) ions are described for two obtained aminophosphonate ligands.     

Synthesis of novel scaffolds based on thiazole or triazolothiadiazine linked to benzofuran or benzo[d]thiazole moieties as new hybrid molecules

Abstract

A synthesis of novel hybrid molecules containing thiazole or bis(thiazoles) each bearing benzofuran and/or benzo[d]thiazole moieties by the reaction of the appropriate thioamide derivatives with the corresponding bis-bromoacetyl derivatives is reported. Mono- and bis(triazolothiadiazine) derivatives based on benzofuran or benzo[d]thiazole moieties were also synthesized in good yields by the reaction of the appropriate bis(bromoacetyl) derivatives with each of 4-amino-5-mercapto-1,2,4-triazoles and their corresponding bis-derivatives.     

Synthesis of oligonucleotides containing thiazole and thiazole N-oxide nucleobases

[reaction: see text] The thiazole C-nucleoside analogue was synthesized by the Hantzsch cyclization method to form the thiazole ring and was then converted to the thiazole N-oxide C-nucleoside analogue by peracid oxidation of the heterocycle nitrogen. Incorporation of the thiazole and thiazole N-oxide phosphoramidites into DNA was successful though significant deoxygenation of the N-oxide occurred during DNA assembly. The mechanism proposed for the reduction of the thiazole N-oxide to thiazole involves the formation of an N-oxide phosphite ester.     

Extending the Substrate Scope of Bicyclic P‐Oxazoline/Thiazole Ligands for Ir‐Catalyzed Hydrogenation of Unfunctionalized Olefins by Introducing a Biaryl Phosphoroamidite Group

This study identifies a series of Ir‐bicyclic phosphoroamidite–oxazoline/thiazole catalytic systems that can hydrogenate a wide range of minimally functionalized olefins (including E‐ and Z‐tri‐ and disubstituted substrates, vinylsilanes, enol phosphinates, tri‐ and disubstituted alkenylboronic esters, and α,β‐unsaturated enones) in high enantioselectivities (ee values up to 99 %) and conversions. The design of the new phosphoroamidite–oxazoline/thiazole ligands derives from a previous successful generation of bicyclic N‐phosphane–oxazoline/thiazole ligands, by replacing the N‐phosphane group with a π‐acceptor biaryl phosphoroamidite moiety. A small but structurally important family of Ir‐phosphoroamidite–oxazoline/thiazole precatalysts has thus been synthesized by changing the nature of the N‐donor group (either oxazoline or thiazole) and the configuration at the biaryl phosphoroamidite moiety. The substitution of the N‐phosphane by a phosphoroamidite group in the bicyclic N‐phosphane–oxazoline/thiazole ligands extended the range of olefins that can be successfully hydrogenated.     

Quaternarisation de l'atome d'azote de systemes tautomeres de la serie des oxo-4 thiazoles. Cycloadditions dipolaires 1,3 des thiazoles mesoioniques formes in situ

4-Hydroxythiazoles and N-acylimino 4-thiazolidinones show similar tautomeric behaviour to azlactones. However, the mechanism of their reaction with dimethylacetylenedicarboxylate or with ethyl vinyl ether differs fundamentally. In the thiazole series, the first step is the quaternization of the nitrogen atom. The mesoionic thiazole intermediate is then trapped by a second molecule of the dipolarophile.     

Dérivés de l'imidazo[2,l-b]thiazole. IX. Comportement du phénacyl-3 dihydro-5,6 imidazo[2,1-b]thiazole et du phénacylidène-3 tétrahydro-2,3,5,6 imidazo[2,1-b]thiazole vis-à-vis du chlorhydrate d'hydroxylamine

The reaction of hydoxylamine hydrochloride with two imidazothiazoles, having a ketonic carbonnyl group, leads to two types of compounds according to the quantity of the sodium acetate used. 3-Phenacyl-5,6-dihydroimidazo[2,1-b]thiazole hydrochloride gives logically the corresponding oxime, isolated in salt form or as a base depending upon the quantity of sodium acetate added. Furbase depending upon the quantity of sodium acetate added. Furthermore, a systematic allylic rearrangement was observed with migration of thiazole double bond to the adjacent nuclear position. 3-Phenacylidene-2,3,5,6-tetrahydroimidazo[2,1-b]thiazole gave directly in the absence of sodium acetate, a rearranged oxime salt. On the other hand, in the presence of sodium acetate, we obtained a hgydroxylamine which was characterized by a double bond in the 2,3-position of the thiazole ring. It is noteworthy that no transformation of the hydroxylamine into the oxime or vice-versa occurs whatever the pH of the solution. These different compounds have no fungistatic activity in contrast to the corresponding ketones.     

Synthesis of trisubstituted thiazoles by ligand-free palladium-catalyzed direct 5-arylation of 2,4-disubstituted thiazoles under conventional and microwave-assisted heating

Trisubstituted thiazoles were synthesized with excellent yields using ligand-free, palladium-catalyzed, direct 5-arylation of 2,4-disubstituted thiazole and conventional or microwave-assisted heating. The palladium-catalyzed reaction yields were significantly influenced by LiCl additive, solvent, and heating method. The reaction times were reduced dramatically by employing microwave radiation instead of conventional heating. The synthetic methods can be applied to diverse 2,4,5-trisubstituted thiazoles by varying the aryl bromide and disubstituted thiazole reactants.     

Biosynthesis of the thiamin-thiazole in eukaryotes: identification of a thiazole tautomer intermediate

Thiamin thiazole biosynthesis in eukaryotes is still not completely understood. In this report, a late intermediate, tightly bound to the active site of the Saccharomyces cerevisiae thiazole synthase, was identified as an adenylated thiazole tautomer. The reactivity of this unusual compound was evaluated. Its identification provides an additional molecular snapshot of the complex reaction sequence catalyzed by the eukaryotic thiazole synthase and identifies the final step of the thiamin-thiazole biosynthesis.     

Reactions of a 4-(trifluoromethyl)thiazole dianion

Treatment of 2-trifluoroacetamido-4-(trifluoromethyl)thiazole with two equivalents of n-butyllithium at -78° produced the thiazole dianion 5 in situ, which reacted preferentially at the 5-position with a variety of electrophiles. These electrophiles include: an aldehyde, ketone, chloroformate, acid chloride, phosphorus oxychloride, silicon chloride, and disulfide. Dianion 5 also combined with dibromodifluoromethane at -98° to give the corresponding 5-(bromodifluoromethyl)thiazole 7 , which is an unusual reaction for an aromatic or heteroaromatic system. Compound 7 was converted to a 4,5-bis-(trifluoromethyl)thiazole 8 using tetrabutylammonium fluoride.     

Etude du mécanisme de la réaction de hantzsch des thiazoles. I. Mise en évidence et détermination des produits intermédiaires et de dégradation

The Hantzsch thiazole synthesis from α-haloketones and thioamides, proceeds via intermediates that can be isolated under certain conditions. These have been identified, mainly by nmr spectroscopy, as thioimidate derivatives. The chain or cyclic structures of these compounds depend upon the nature of the substituents. Their dehydration gives together with the expected thiazole, secondary products which have also been isolated and identified as α-mercaptoketones and α-ketothiolesters.     

Bromination of 4-(2-thienyl)thiazoles and 2-(2-thienyl)quinoline

Depending on the substituent, the bromination of 4-(2-thienyl)thiazoles and 2-(2-thienyl)quinoline takes place in the 5 position of the thiophene or thiazole ring. When an amino group is present in the 2 position of the thiazole ring, bromination takes place in the 5 position of the thiazole ring. When excess brominating agent is present, a second bromine atom enters the 5 position of the free ring.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 1, pp. 35–38, January, 1982.     

The Chiral Synthesis of Thiazole Amino Acid Enantiomers

An efficient modified Hantzsch reaction is described for the synthesis of optically pure thiazole amino acid derivatives from the corresponding amino acids. The method is exemplified by the synthesis of a derivative of L-(Gln)Thz, the novel chiral thiazole amino acid moiety of dolastatin 3. The Cotton effects of thiazole amino acids correlate well with the absolute stereochemistry of these compounds.     

Polymethine dyes — Indolo[3,2-d]thiazole derivatives

New polymethine dyes with an indolo[3,2-d]thiazole residue are described, and their spectral properties are discussed. Replacement of the vinylene group in the naphtho[1,2-d]thiazole residue by an NH group leads to a considerably greater bathochromic shift of the absorption maximum of carbo- and merocyanines as compared with replacement by a sulfur atom. The basicity of the indolo[3,2-d]thiazole residue is higher than the basicity of the naphtho[1,2-d]-thiazole and thionaphtheno[3,2-d]thiazole residues.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 12, pp. 1606–1610, December, 1972.     

A base induced fragmentation of tetramisole

The exposure of dl-2,3,5,6-tetrahydro-6-phenylimidazo[2,1-6 Jthiazole (tetramisole) to lithium diisopropylamide in tetrahydrofuran ruptures the thiazole ring to give, following the introduction of primary or secondary alkyl halides, 1-(2′-alkylthio)ethyl-4-phenylimidazoles. Conclusive evidence for the thiazole ring opening was obtained by a single crystal x-ray diffraction study of 1-(2′-p-bromobenzylthio)ethyl-4-phenylimidazole.     

Stereoselective synthesis of highly functionalized thiopeptide thiazole fragments from uronic acid/cysteine condensation products: access to the core dipeptide of the thiazomycins and nocathiacins

We present the stereoselective synthesis of various highly functionalized thiazole dipeptides that are found in thiopeptide antibiotics like thiazomycins and nocathiacins. The condensation of an uronic acid with l-cysteine methyl ester delivers along two different protocols the stereopure thiazolidine lactones or lactams on the multigram scale, respectively. Oxidation of the thiazolidine moiety to the thiazole and tailoring of the sugar chains yield the thiazole dipeptide as present in the core motif of the thiopeptide antibiotics, as well as its epimer and a homolog. The modular assembly of the potent natural products and their analogs relies on the synthetic accessibility of adequately protected building blocks of tailored absolute stereochemistry.     

Research on benz- and naphthazoles

The synthesis of 2-hydrazinonaphth[2, 1-d]thiazole is effected, and its ability to undergo autoxidation in ethanol solution to give 1, 5-di(naphth[2, 1-d]thiazolyl-2)-3-methylformazan is established. Unsymmetrical 1-naphth[2, 1-d]thiazolyl-5-tolyl-3-aryl(or methyl) formazans are obtained by coupling a p-tolyldiazonium compound with the appropriate 2-hydrazinonaphth[2, 1-d]thiazole hydrazones.For Part XIX see [3].     

Theoretical Study on Second‐order Nonlinear Optical Properties of Substituted Thiazole Derivatives

On the basis of ZINDO program, we have designed a program to calculate the nonlinear second‐order polarizability β_yk and β_μ according to the SOS expression. The second‐order nonlinear optical properties of 4‐nitro‐4′‐dimethylamino‐stilbene and a series of its thiazole derivatives were studied. The calculated results were that: When replacing a benzene ring in 4‐nitro‐4′‐dimethylamino‐stilbene by a thiazole ring, the influence on β values depends on the position of thiazole ring. When the thiazole ring connects with nitro group (acceptor), the β values increase significantly compared with corresponding stilbene derivatives. The β values of 2‐(p‐donor‐β‐styryl)‐5‐nitro‐thiazole derivatives (2–7) are larger than those of 2‐(p‐nitro‐β‐styryl)‐5‐donor‐thiazole derivatives (8–13) and 2‐(p‐donor‐phenyl)‐azo‐5‐nitro‐thiazole derivatives (14–19). The 2‐(p‐donor‐β‐styryl)‐5‐nitro‐thiazole derivatives (2–7) are good candidates as chromophores duo to their high nonlinearities and potential good thermal stability.     

Concise assembly of highly substituted furan-fused 1,4-thiazepines and their Diels-Alder reactions with benzynes

A facile and highly efficient three-component reaction of thiazole or benzothiazole carbenes, disubstituted ketenes, and activated alkynes is disclosed. With this methodology, a polysubstituted ring system containing furo[2,3-c]thiazepine core can be constructed from simple and readily accessible starting materials in good yields. The scope and limitation of this transformation were investigated in detail by using various thiazole carbene, ketene, and alkyne components. Furthermore, the synthetic utilities of these unique polyheterocyclic compounds were demonstrated via their Diels-Alder reactions with benzynes to furnish thiazepine-fused 7-oxanorbornadiene derivatives in excellent yields.     

Concerning the preparations of some pyridylimidazothiazole derivatives

The preparations of some 4-pyridylimidazo[2,1-b]thiazole and -imidazo[5,1-b]thiazole derivatives are described. In some of the cyclizations to form the imidazothiazole ring systems, trifluoroacetic anhydride, the dehydration reagent employed, participated in the reaction leading to products bearing a trifluoromethyl or trifluoroacetyl substituent.     

Syntheses of aromatic substituted hydrazino-thiazole derivatives to clarify structural characterization and antioxidant activity between 3-arylsydnonyl and aryl substituted hydrazino-thiazoles

This work clarifies the structural characterization and antioxidant activity between aromatic and 3-arylsydnonyl substituted hydrazino-thiazoles by further synthesizing a series of aromatic ring-substituted hydrazino-thiazole derivatives 8a-h and 9a-h. Hydrazino-thiazole derivatives 8a-h and 9a-h were obtained by reacting aromatic or heterocyclic aromatic aldehyde thiosemicarbazones 7a-h with cyclization reagents ethyl 2-chloroacetoacetate (2a) and 2-bromoacetophenone (2b), respectively. The ORTEP drawings of compounds 8g, 8h and 9f provide strong evidence of the structure of aromatic thiazole derivatives 8a-h and 9a-h. Undoubtedly, the structure of compounds 3e-h and 4e-h synthesized by the reaction of 3-aryl-4-formylsydnone thiosemicarbazones 1e-h with cyclization reagents 2a and 2b in the previous work should have the thiazole moiety, and not the thiazoline moiety. Both the new thiazole derivatives 8a-h and 9a-h and the 3-arylsydnonyl-substituted derivatives 3e-h and 4e-h were investigated to determine their antioxidant activity by two tests that have been highly documented-the direct scavenging effect on a stable free 1,1-diphenyl-2-picrylhydrazyl (DPPH) radical and the inhibition of the 2,2-azino-bis(3-ethylbenzthiazoline-6-sulfonic acid) (ABTS) radical. Results of this study demonstrate that not only the thiazole ring and the aryl ring has the contribution to the antioxidant activities, the sydnone ring of 3-arylsydnonyl moiety also has its considerable contribution.