Synthesis of novel C6-phosphonated purine nucleosides under microwave irradiation by SNAr-Arbuzov reaction

Novel C6-phosphonated purine nucleosides were obtained in good to excellent isolated yields by the simple and catalyst-free SNAr-Arbuzov reaction of trialkyl phosphite with 6-choloropurine nucleosides, including a series of nonsugar carbon nucleosides. Shorter reaction times were needed, and substantially higher yields were obtained under microwave irradiation conditions compared with conventional heating conditions.     

Analogs of purine nucleosides and purine mono-and polynucleotides

A number of 6-substituted 9-(1,5-dihydroxy-3-pentyl)purines were obtained from 5-amino-4,6-dichloropyrimidine. 5-Amino-4,6-dichloropyrimidine reacts with 2-hydroxymethylpyrrolidine to give 4-chloro-5-amino-6-(2-hydroxymethylpyrrolidino)pyrimidine.See [1] for communication IV.Deceased.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 4, pp. 552–555, April, 1976.     

The first direct C-H arylation of purine nucleosides

Pd-catalyzed direct C-H arylation of unprotected purine nucleosides with aryl iodides at position 8 was developed to allow a straightforward single-step introduction of diverse aryl groups.     

Analogs of purine nucleosides and purine mono- and polynucleotides

On the basis of a comparison of the protolysis constants and vibrational frequencies it is shown that intermolecular interactions are present in 6-substituted 9-(,-dihydroxyalkyl)-purines and the corresponding mono- and diphosphates. In addition, in the case of the phosphates the existence of intramolecular interactions of electrostatic character between the phosphate group and the heteroring is also proposed. A comparison of the protolysis constants provides evidence for the different character of the interaction of the dihydroxyalkyl residue with the heteroring of the base in series of adenine and hypoxanthine derivatives.See [1] for communication II.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 12, pp. 1684–1689, December, 1974.     

Total synthesis of 3',5'-C-branched nucleosides

[reaction: see text] A novel total synthesis of 3',5'-C-branched uridine azido acid has been accomplished using stereoselective aldehyde alkynylation, Ireland-Claisen rearrangement, and iodolactonization as the key reactions. Compared to traditional routes that start from carbohydrates, the present methodology is more efficient, flexible for future optimization, and provides access to both enantiomers of the products. Because the key chemistry does not involve the 3'- and 5'-C substituents, our route is a general approach to 3',5'-C alkyl nucleoside analogues.     

Analogs of purine nucleosides and purine mono- and polynucleotides

Selective protection of the amino and one of the hydroxyl groups of 6-substituted 9-(α,ω-dihydroxy-2-alkyl)purines was realized. A convenient method for the preparation of monophosphates was developed.     

Analogs of purine nucleosides and purine mono- and polynucleotides

Phosphorylation of 6-substituted 9-(1, 5-dihydroxy-3-pentyl)purines with 2-cyanoethyl phosphate in the presence of dicyclohexylcarbodiimide in anhydrous pyridine gave their 1, 5-diphosphates. Oligomers containing pyrophosphate and ester bonds were obtained by polycondensation of 1, 5-diphosphates of 6-dimethylamino- and 6-oxo-9-(1, 5-dihydroxy-3-pentyl)purines with the appropriate 9-(1, 5-dihydroxy-3-pentyl) purines.See [1] for communication V.Deceased.Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 5, pp. 693–696, May, 1976.     

Chemical synthesis of cross-linked purine nucleosides

[reaction: see text] An efficient route to all of the possible cross-linked 2'-deoxypurines 1-3 has been developed by means of the Pd-mediated C-N bond formation in the key step. Utilizing this protocol, the synthesis of the first unnatural protected purine trimeric adduct 4 has been accomplished.     

Synthesis of some 3',5'-dideoxy-5'-C-phosphonomethyl nucleosides.

Ammonium [1-(3',5',6'-trideoxy-beta-D-erythro-hexofuranosyl)thymine]-6'- phosphonate (1), ammonium 3',5'-dideoxycytidine-5'-C-methylphosphonate (2) and 3',5'-dideoxyadenosine-5'-C-methyl phosphonic acid (3) have been synthesized and tested for anti-HIV activity. The key steps involved an Arbuzov reaction between triethyl phosphite and 3,5,6-trideoxy-6-iodo-1,2-O-isopropylidene-alpha-D-erythro- hexofuranose (7), followed by condensation with the appropriate nucleoside bases. The substances 1, 2 and 3 have been tested in vitro against HIV.     

Voltammetric studies of purine bases and purine nucleosides with copper

Anodic stripping voltammetry with a hanging mercury drop electrode has been used to investigate the interaction of cooper with the purines adenine, hypoxanthine, xanthine and purine nucleosides adenosine, guanosine and inosine at an ionic strength of 0.1 M in KNO₃ and in the pH range 3.5–5.5. In all cases stabilisation of copper(I) occurs suggesting that the oxidation of copper(0) in the presence of excess ligand proceeds in two one-electron steps.Adsorption onto the electrode has been analysed and conditions where this is negligible were chosen for complexation studies. From the shift of the peak potential corresponding to Cu(0)/Cu(I) oxidation with increasing ligand concentration the stoichiometry of the complexes and their formation constants have been determined. The values obtained are discussed in terms of the ligand structure.     

An efficient and green preparation of 5-aminophosphonate substituted pyrimidine nucleosides under solvent-free conditions

<正>An environmentally benign and highly efficient one-pot preparation ofα-aminophosphonates under solvent-free conditions was developed.By employing this method,5-aminophosphonate substituted pyrimidine nucleosides were synthesized in good to excellent yields starting from 5-formyl-2'-deoxyuridine,aniline and dimethylphosphite.     

Acyclic analogues of purine and imidazole nucleosides

Hydroxyl-protected derivatives of 1- and 3-(2-hydroxyethoxymethyl)imidazoles ( 4,5,7-10 ) have been prepared from 5-amino-4-carbamoylimidazoles ( 2 ). The protected derivatives were converted to acyclic analogues of imidazole nucleosides ( 6 ) or subjected to various cyclisation reactions leading to 9-(2-hydroxy-ethoxymethyl)-substituted 2-methyl-, 2-phenyl- and 2-azahypoxanthines ( 18,13 and 20 , respectively) and 1-methylguanine ( 28 ). For assignment of structures to isomeric imidazole and purine derivatives, ¹³C chemical shifts have been used.     

Model studies of DNA C5' radicals. Selective generation and reactivity of 2'-deoxyadenosin-5'-yl radical

The reaction of hydrated electrons (e(aq)(-)) with 8-bromo-2'-deoxyadenosine has been investigated by radiolytic methods coupled with product studies and addressed computationally by means of DFT-B3LYP calculations. Pulse radiolysis revealed that this reaction was complete in approximately 0.3 mus, and, at this time, no significant absorption was detected. The spectrum of a transient developed in 20 mus has an absorbance in the range 300-500 nm (epsilon(max) congruent with 9600 M(-1) cm(-1) at 360 nm), and it was assigned to aromatic aminyl radical 3. Computed vertical transitions (TD-UB3LYP/6-311+G) are in good agreement with the experimental observations. Radical 3 is obtained by the following reaction sequence: one-electron reductive cleavage of the C-Br bond that gives the C8 radical, a fast radical translocation from the C8 to C5' position, and an intramolecular attack of the C5' radical at the C8,N7 double bond of the adenine moiety. The rate constant for the cyclization is 1.6 x 10(5) s(-1). On the basis of the theoretical findings, the cyclization step is highly stereospecific. The rate constants for the reactions of C5' and aminyl 3 radicals with different oxidants were determined by pulse radiolysis methods. The respective rate constants for the reaction of 2'-deoxyadenosin-5'-yl radical with dioxygen, Fe(CN)(6)(3)(-), and MV(2+) in water at ambient temperature are 1.9 x 10(9), 4.2 x 10(9), and 2.2 x 10(8) M(-1) s(-1). The value for the reaction of aminyl radical 3 with Fe(CN)(6)(3-) is 8.3 x 10(8) M(-1) s(-1), whereas the reaction with dioxygen is reversible. Tailored experiments allowed the reaction mechanism to be defined in some detail. A synthetically useful radical cascade process has also been developed that allows in a one-pot procedure the conversion of 8-bromo-2'-deoxyadenosine to 5',8-cyclo-2'-deoxyadenosine in a diastereoisomeric ratio (5'R):(5'S) = 6:1 and in high yield, by reaction with hydrated electrons in the presence of K(4)Fe(CN)(6).     

Addition of difluorocarbene to 4',5'-unsaturated nucleosides: synthesis and deoxygenation reactions of difluorospirocyclopropane nucleosides

Synthetic routes to 4'-(2,2-difluorospirocyclopropane) analogues of adenosine, cytidine, and uridine are described. Treatment of 2',3'-O-isopropylidene-4',5'-unsaturated compounds derived from adenosine and uridine with difluorocarbene (generated from PhHgCF3 and NaI) gave diastereomeric mixtures of the 2,2-difluorospirocyclopropane adducts. Stereoselectivity resulting from hindrance by the isopropylidene group favored addition at the beta face. Removal of base and sugar protecting groups gave new difluorospirocyclopropane nucleoside analogues. The protected uridine analogue was converted into its cytidine counterpart via a 4-(1,2,4-triazol-1-yl) intermediate. Stannyl radical-mediated deoxygenation of the 3'-O-TBS-2'-thionocarbamate derivatives gave the 2'-deoxy products of direct hydrogen transfer. In contrast, identical treatment of the 2'-O-TBS-3'-thionocarbamate isomers resulted in opening of the vicinal difluorocyclopropane ring upon generation of a C3' radical followed by homoallylic hydrogen transfer to give 4'-(1,1-difluoroethyl)-3',4'-unsaturated nucleoside derivatives. Structural aspects and biological effect considerations are discussed.