Showing papers on "Bicyclic molecule published in 1996"
TL;DR: In this article, a bicyclo[310]hexane template was used to fix the ring pucker of 2'-deoxy-methanocarba-nucleosides to values corresponding to either one of these two extreme conformations that are typical of nucleosides.
Abstract: The sugar moiety of nucleosides in solution is known to exist in a rapid dynamic equilibrium between extreme Northern and Southern conformations as defined in the pseudorotational cycle In the present work, we describe how the bicyclo[310]hexane template fixes the ring pucker of 2‘-deoxy-methanocarba-nucleosides 1−5 and 12 to values corresponding to either one of these two extreme conformations that are typical of nucleosides The syntheses of the fixed Northern conformers 1−5 were performed by Mitsunobu coupling of the heterocyclic bases with the chiral carbocyclic alcohol 6 [(1R,2S,4R,5S)-1-[(benzyloxy)methyl]-2-(tert-butyloxy)-4-hydroxybicyclo[310]hexane], while the synthesis of the Southern conformer, (S)-methanocarba-T (12), was reported earlier Carbocyclic thymidine (carba-T, 13) was used as a reference, flexible carbocyclic nucleoside Antiviral evaluation of these compounds revealed a very potent antiherpetic activity associated with the Northern thymidine analogue 2, which was more powerful
248 citations
TL;DR: Ruthenium alkylidene 1 has been utilized in the tandem ring opening−ring closing metathesis of cyclic olefins as mentioned in this paper, where reactivity is dependent upon strain and thus ring size, in the substrate molecules.
Abstract: Ruthenium alkylidene 1 has been utilized in the tandem ring opening−ring closing metathesis of cyclic olefins. This reaction produces a bicyclic molecule from a cyclic olefin. Reactivity is dependent upon strain, and thus ring size, in the substrate molecules. Competing oligomerization is observed in substrates having low ring strain; this process is inhibited by increasing dilution of the reaction or by adding alkyl substitution to the acyclic olefins.
208 citations
189 citations
TL;DR: A novel pyridinium salt photoelectrocyclization-nucleophilic bicyclic aziridine ring opening reaction sequence has been investigated in order to determine its preparative potential, yielding trans,trans-trisubstituted cyclopentenes exclusively.
Abstract: A novel pyridinium salt photoelectrocyclization−nucleophilic bicyclic aziridine ring opening reaction sequence has been investigated in order to determine its preparative potential. N-Alkylpyridinium perchlorates were found to undergo photoinduced electrocyclization upon irradiation in nucleophilic solvents, such as H2O and MeOH, to efficiently produce 6-alkyl-6-azabicyclo[3.1.0]hex-2-en-4-yl alcohols and ethers. The bicyclic aziridine photoproducts react with a number of different nucleophiles (e.g., H2O, MeOH, AcOH, AcSH) under acid-catalyzed conditions to produce 5-(nucleophile-substituted)-4-(alkylamino)cyclopenten-3-yl alcohols and ethers. The aziridine ring opening processes are both regioselective and stereoselective, yielding trans,trans-trisubstituted cyclopentenes exclusively, apparently as a consequence of the operation of an SN2 mechanism. The effects of C-alkyl substitution on the regiochemistry of the pyridinium cation photocyclization reaction were briefly probed, and a method was developed...
184 citations
TL;DR: In this paper, Pd(II)-catalyzed homo-and copolymerizations of norbornene derivatives were obtained by cycloaliphatic polyolefins with functional groups.
Abstract: Cycloaliphatic polyolefins with functional groups were obtained by Pd(II)-catalyzed homo- and copolymerizations of norbornene derivatives. Bicyclo[2.2.1]hept-5-ene-2-carboxylic acid, the corresponding methyl ester, 2-(hydroxymethyl)bicyclo[2.2.1]hept-5-ene, and the corresponding octanoate and decanoate were used as the monomers in these addition polymerizations. Pd(II)−nitrile catalysts [Pd(RCN)4][BF4]2 (with R = CH3 and C2H5) quite selectively polymerized the exo isomers of the esters of 2-(hydroxymethyl)bicyclo[2.2.1]hept-5-ene. Monomer mixtures containing an 80/20 ratio of endo/exo isomers were converted into polymers containing more than 50% of exo units. 1H NMR studies showed that the predominant fraction of the endo isomer remained unreacted. The nitrile based Pd catalysts were not sufficiently active to polymerize the monomers with electron-withdrawing substituents linked to the bicyclic unit at ambient temperature. In-situ prepared (η3-allyl)palladium complexes with associated tetrafluoroborate an...
158 citations
TL;DR: From these compounds, 20, 21, 22, 23, 28, and 34 showed a specific activity against cytomegalovirus and/or varicella-zoster virus.
Abstract: The synthesis and the antiviral activities of C-3 acyclic nucleoside analogues of imidazo[1,2-a]pyridine and pyrimidine are reported. From these compounds, 20, 21, 22, 23, 28, and 34 showed a specific activity against cytomegalovirus and/or varicella-zoster virus.
144 citations
TL;DR: In this paper, the reaction of 2-allylanilines with CO/H2 using the catalytic system Pd(OAc)2/PPh3, while use of 1,4-bis(diphenylphosphino)butane instead of PPh3 in the latter process results in the formation of the seven-membered ring lactams benzazepinones in good yield.
Abstract: 2-Allylphenols react with carbon monoxide and hydrogen in the presence of catalytic quantities of a cationic palladium(II) complex [(PCy3)2Pd(H)(H2O)]+BF4- or palladium acetate and 1,4-bis(diphenylphosphino)butane, affording five- or seven-membered ring lactones (bicyclic, tricyclic, and pentacyclic) as the principal products, often in excellent yields. Use of 2-aminostyrenes as reactants and catalytic quantities of palladium acetate and tricyclohexylphosphine, affords five-membered ring lactams in high yield and selectivity. Bicyclic and tricyclic heterocycles containing six-membered ring lactams can be synthesized from the reaction of 2-allylanilines with CO/H2 using the catalytic system Pd(OAc)2/PPh3, while use of 1,4-bis(diphenylphosphino)butane instead of PPh3 in the latter process results in the formation of the seven-membered lactams benzazepinones in good yield. The regiochemical control depends on the nature of the palladium catalyst, the relative pressures of the gases, and the solvent.
143 citations
134 citations
TL;DR: In this article, the authors performed ab initio molecular orbital calculations on nine bridgehead bicyclic lactams ranging from the 2.2 to the 4.3 series and found that the smaller lactams were N-protonated, the larger O-proptonated, and the crossover was predicted to occur around the 3.3.
Abstract: Optimized ab initio molecular orbital calculations on nine bridgehead bicyclic lactams ranging from the 2.2.2 to the 4.3.3 series indicate variations in structural properties, resonance energies, proton affinities, and core orbital ionization energies that reflect the trans-cycloalkene analogy. The smaller lactams are calculated to be N-protonated, the larger O-protonated, and the “crossover” is predicted to occur around the 3.3.1 system. On the basis of resonance energies, larger bridgehead bicyclic lactams could be considered to be hyperstable as Schleyer and co-workers define the concept for larger bridgehead alkenes. This, hyperstability should be apparent in the kinetics of the nucleophilic substitution reactions of the lactams, such as hydrolysis, but not in the thermochemistry of these reactions.
128 citations
TL;DR: A broad screening of phytochemicals has demonstrated that certain flavone and flavonol derivatives have a relatively high affinity at A3 adenosine receptors, and these series of flavonoids provide leads for the development of novel potent and subtype selective A3 antagonists.
Abstract: A broad screening of phytochemicals has demonstrated that certain flavone and flavonol derivatives have a relatively high affinity at A3 adenosine receptors, with Ki values of > or = 1 microM (Ji et al. J. Med. Chem. 1996, 39, 781-788). We have further modified the flavone structure to achieve a degree of selectivity for cloned human brain A3 receptors, determined in competitive binding assays versus [125I]AB-MECA[N6-(4-amino-3-iodobenzyl)adenosine-5'-(N-methylur onamide)]. Affinity was determined in radioligand binding assays at rat brain A1 and A2a receptors using [3H]-N6-PIA ([3H]-(R)-N6-phenylisopropyladenosine) and [3H]CGS21680 [[3H]-2-[[4-(2-carboxyethyl)phenyl]ethylamino]-5'-(N-ethylcarbamoyl++ +)adenosine], respectively. The triethyl and tripropyl ether derivatives of the flavonol galangin, 4, had Ki values of 0.3 - 0.4 microM at human A3 receptors. The presence of a 5-hydroxyl group increased selectivity of flavonols for human A3 receptors. The 2',3,4',7-tetraethyl ether derivative of the flavonol morin, 7, displayed a Ki value of 4.8 microM at human A3 receptors and was inactive at rat A1/A2a receptors. 3,6-Dichloro-2'-(isopropyloxy)-4'-methylflavone, 11e, was both potent and highly selective (approximately 200-fold) for human A3 receptors (Ki = 0.56 microM). Among dihydroflavonol analogues, the 2-styryl instead of the 2-aryl substituent, in 15, afforded selectivity for human A3 vs rat A1 or A2A receptors. The 2-styryl-6-propoxy derivative, 20, of the furanochromone visnagin was 30-fold selective for human A3 receptors vs either rat A1 or A2A receptors. Several of the more potent derivatives effectively antagonized the effects of an agonist in a functional A3 receptor assay, i.e. inhibition of adenylyl cyclase in CHO cells expressing cloned rat A3 receptors. In conclusion, these series of flavonoids provide leads for the development of novel potent and subtype selective A3 antagonists.
111 citations
Patent•
Icos1
TL;DR: In this article, a compound of formula (I) and solvates thereof, in which R0 represents hydrogen, halogen or C?1-6?alkyl; R?1? represents hydrogen or c?1 -6 -alkyl, R?2? represents the bicyclic ring (1) which may be optionally substituted by one or more groups selected from halogen and C? 1-3 -3-alkyl.
Abstract: A compound of formula (I) and solvates thereof, in which R0 represents hydrogen, halogen or C?1-6?alkyl; R?1? represents hydrogen or C?1-6?alkyl; R?2? represents the bicyclic ring (1) which may be optionally substituted by one or more groups selected from halogen and C?1-3?alkyl; and R?3? represents hydrogen or C?1-3?alkyl A compound of the present invention is a potent and selective inhibitor of cGMP specific PDE having a utility in a variety of therapeutic areas where such inhibition is beneficial
TL;DR: In this paper, the synthesis of dihydropyrroles, pyrrole, and indoles through [3-atom + 2-atom] combination of ethyl or aryl tosylamide anions with phenyl(propynyl)iodonium triflate is described.
Abstract: The synthesis of dihydropyrroles, pyrroles, and indoles through [3-atom + 2-atom] combination of ethyl or aryl tosylamide anions with phenyl(propynyl)iodonium triflate, and the base-mediated intramolecular bicyclization of alkynyliodonium-bearing tosylamide or tosylimide substrates to furnish bicyclic and tricyclic tosylenamide (-enimide) products, is described. A detailed discussion of the scope, limitations, byproduct formation, and the basis for observed diastereoselectivity is presented.
TL;DR: In this paper, a radical mechanism was used to obtain a (tetrahydrofuranylmethyl)zinc halide of type 1, which can be reacted with various electrophiles after a transmetalation with CuCN·2LiCl.
Abstract: Unsaturated iodo or bromo acetals of type 2 undergo a smooth cyclization mediated by diethylzinc (2 equiv) and Ni(acac)2 as catalyst (2−5 mol %). These cyclizations proceed via a radical mechanism affording a (tetrahydrofuranylmethyl)zinc halide of type 1, which can be reacted with various electrophiles after a transmetalation with CuCN·2LiCl. High stereoselectivities are usually observed in the ring closures, especially if monocyclic cyclization precursors are used. In these cases, bicyclic products of the endo-configuration are obtained with over 94% diastereoselectivity. The synthetic method has been extended to the preparation of a nitrogen heterocycle and over 98% pure trans-4,5-disubstituted γ-butyrolactones. A short enantioselective synthesis of (−)-methylenolactocine (3) using the radical cyclization and a novel oxidation of α-silyl zinc peroxide as a key step is also described.
TL;DR: Highly 5-HTT selective agents such as 5 and 6 may be useful as brain-imaging ligands for serotonin neurons or as mood-elevating drugs, while the high affinity and selectivity for the DA transporter found in N-(fluoropropyl)-2 beta-carboxymethoxy-3 bet-(4'-iodophenyl)nortropane (FP-beta-CIT, 5) support their use as improved markers for DA neurons.
Abstract: This report concerns the synthesis and chemical characterization of novel series of N-substituted 2 beta-carbomethoxy-3 beta-(4'-iodophenyl)tropane (beta-CIT, 2) analogs and their neuropharmacological evaluation for affinity at dopamine (DAT), serotonin (5-HTT), and norepinephrine membrane transporters in rat brain tissue. N-Substituted analogs of beta-CIT with a 2 beta-carbomethoxy ester moiety showed lower DAT affinity than beta-CIT for the DAT, and some were more selective for the 5-HTT over the DAT. 2 beta-Carbomethoxy(iodophenyl)nortropane analogs of beta-CIT with the N-substituents difluoroethyl, mesoxypropyl, iodopropyl, and methylpropionyl all yielded > 10-fold lower DAT affinity than beta-CIT itself, whereas the N-(fluoropropyl)-2 beta- isopropyl ester analog (1) of beta-CIT exceeded beta-CIT (2, an N-methyl-2 beta-carbomethoxy ester) in DAT affinity. Several N-haloalkyl-substituted beta-CIT analogs yielded high 5-HTT affinity (Ki N-chloropropyl (4) > or = N-bromopropyl (3) > beta-CIT (2) > N-3'-phtalimidopropyl (11), with particularly high (ca. 30-fold) 5-HTT-over-DAT selectivity found in the N-fluoropropyl (5) and N-fluoroethyl (6) compounds, compared to only 3.o-fold 5-HTT selectivity in beta-CIT itself. Highly 5-HTT selective agents such as 5 and 6 may be useful as brain-imaging ligands for serotonin neurons or as mood-elevating drugs, while the high affinity and selectivity for the DA transporter found in N-(fluoropropyl)-2 beta-(carboxyisopropyl)-3 beta-(4'-iodophenyl)-nortropane (1) and N-(fluoropropyl)-2 beta-carboxymethoxy-3 bet-(4'-iodophenyl)nortropane (FP-beta-CIT, 5) support their use as improved markers for DA neurons.
TL;DR: Two novel series of 2-pyridones were synthesized by transposition of the nitrogen of 4-quinolones to the bridgehead position which yielded two novel heterocyclic nuclei, pyrido[1,2-alpha]pyrimidine and quinolizine, which had not previously been evaluated as antibacterial agents and were found to be potent inhibitors of DNA gyrase.
Abstract: Two novel series of 2-pyridones were synthesized by transposition of the nitrogen of 4-quinolones to the bridgehead position. This subtle interchange of the nitrogen atom with a carbon atom yielded two novel heterocyclic nuclei, pyrido[1,2-a]pyrimidine and quinolizine, which had not previously been evaluated as antibacterial agents and were found to be potent inhibitors of DNA gyrase. Quinolizines with a methyl group at the 9-position such as (S)-45a (ABT-719) demonstrate exceptional broad spectrum antibacterial activity. Most notably, they are active against resistant bacteria such as methicillin-resistant Staphylococcus aureus, vancomycin-resistant strains of enterococci, and ciprofloxacin-resistant organisms. In addition, 2-pyridones also possess favorable physiochemical and pharmacokinetic properties. These 2-pyridones were synthesized from the commercially available starting materials by 10−17 linear transformations. The structure of an adduct yielded by this sequence, (S)-45a (ABT-719), was determin...
TL;DR: In this article, β-Lactams were synthesized by the carbonylative ring expansion of aziridines catalyzed by dicobalt octacarbonyl under CO pressure.
Abstract: β-Lactams were synthesized by the carbonylative ring expansion of aziridines catalyzed by dicobalt octacarbonyl under CO pressure. The active catalyst, cobalt tetracarbonyl anion, induces nucleophilic ring opening of the heterocycle, resulting in inversion of configuration. The regio- and stereospecificity of this reaction resulted in the synthesis of the first highly strained trans-7-azabicyclo[4-2-0]octan-8-one derivatives.
Patent•
18 Jan 1996TL;DR: In this paper, the authors proposed a method for the inhibition of platelet aggregation using six membered rings of a bicyclic compound, such as benzopyran, iso-quinoline, isoquinoline or tetrahydronaphthalene.
Abstract: This invention relates to certain bicyclic compounds having a nucleus formed of two fused six membered rings, for example, benzopyran, isoquinoline, isoquinolone, tetrahydronaphthalene, dihydronaphthalene, or tetralone, substituted with both basic and acidic functionality, which are useful in inhibition of platelet aggregation.
TL;DR: No further enhancement of the selectivity of the benzazepine ring system could be obtained via introduction of a second heteroatom (N, O, S) at the 5-position in this ring system.
Abstract: In the search for potent and selective inhibitors of the enzyme phenylethanolamine N-methyltransferase (PNMT; EC 2.1.1.28), we examined the effect of ring size or an additional heteroatom in the conformationally-restricted benzylamine-type PNMT inhibitors. Based on semiempirical calculations (MNDO) and molecular modeling studies, PNMT-inhibitory activity of these compounds seemed to be dependent on (a) the torsion angle between the plane of the aromatic ring and the endo N atom lone pair ( tau 2 angle), with the optimal value of tau 2 being about - 75 degrees, and (b) the amount of steric bulk about the 3-position of 1,2,3,4-tetrahydroisoquinoline (5, THIQ). 2,3,4,5-Tetrahydro-1H-2-benzazepine (6) was found to have the highest selectivity (PNMT Ki = 3.34 microM, alpha 2 Ki = 11 microM, selectivity = 3.2) as compared to other homologues of THIQ (PNMT Ki = 9.67 microM, alpha 2 Ki = 0.35 microM, selectivity = 0.036). The higher PNMT-inhibitory activity of 6 was attributed to favorable steric interactions of the puckered methylene groups in the putative bioactive conformation of 6 at the PNMT active site, whereas unfavorable interactions of these puckered methylene groups at the alpha 2-adrenoceptor were thought to be the cause of reduced alpha 2 affinity of 6. No further enhancement of the selectivity of the benzazepine ring system could be obtained via introduction of a second heteroatom (N, O, S) at the 5-position in this ring system.
TL;DR: A series of substituted monocyclic and bicyclic azepinones were incorporated as di peptide surrogates in mercaptoacetyl dipeptides with the desire to generate a single compound which would potently inhibit both angiotensin-converting enzyme (ACE) and neutral endopeptidase (NEP).
Abstract: A series of substituted monocyclic and bicyclic azepinones were incorporated as dipeptide surrogates in mercaptoacetyl dipeptides with the desire to generate a single compound which would potently inhibit both angiotensin-converting enzyme (ACE) and neutral endopeptidase (NEP). Many of these compounds displayed excellent potency against both enzymes. Two of the most potent compounds, monocyclic azepinone 2n and bicyclic azepinone 3q, demonstrated a high level of activity versus ACE and NEP both in vitro and in vivo.
TL;DR: In this article, a bioassay-guided fractionation of the EtOAc extract of sponge Plakortis halichondrioides yielded four bicyclic lactones, plakortones A, B, C, D, and a novel acid, PLAKortide E ( 3, 4, 5, 6 and 7 ).
TL;DR: In this paper, the reaction of 5-hexenyl iodides with diethylzinc (2 equiv) and catalytic amounts of a PdII or NiII complex like PdCl2(dppf) or Ni(acac)2 results in an efficient ring closure (THF, RT, 2-12 h) affording cyclopentylmethylzinc iodides, which, after transmetalation with CuCN·2LiCl, can be further functionalized by treatment with a range of electrophiles like allylic halides
Abstract: The reaction of 5-hexenyl iodides with diethylzinc (2 equiv) and catalytic amounts of a PdII or NiII complex like PdCl2(dppf), PdCl2(MeCN)2, or Ni(acac)2 results in an efficient ring closure (THF, RT, 2–12 h) affording cyclopentylmethylzinc iodides, which, after transmetalation with CuCN·2LiCl, can be further functionalized by treatment with a range of electrophiles like allylic halides, acyl chlorides, enones, nitroolefins, ethyl propynoate, and alkynyl halides to yield polyfunctional cyclopentane derivatives. The ring closures occur via radical intermediates, and the stereochemistry of the products can be explained according to the rules for radical cyclizations developed by Beckwith. The preparation of several di- and trisubstituted cyclopentanes has been achieved with high stereoselectivity. Tandem ring closures can be performed to construct bicyclic or tricyclic ring systems. Cyclizations of iodo-ethylenic and acetylenic esters and ketones can be accomplished, although the high reactivity of acetylenic ketones leads to unexpected cyclization products. The synthetic utility of this method has been demonstrated by an enantioselective synthesis of (+)-methyl epijasmonate and (-)-methyl cucurbate.
TL;DR: The preparation of the unnatural bicyclic alpha-amino acids 7 and 8 is described along with their utility as chiral ligands in the copper-catalyzed enantioselective allylic oxidation of cylohexene.
TL;DR: In marked contrast to the ribosylbenzimidazoles, none of the acyclic analogs were specific and potent inhibitors of HCMV.
Abstract: The sodium salt of 2,5,6-trichlorobenzimidazole (8a) was condensed with [2-(benzyloxy)ethoxy]-methyl chloride (9) and [1,3-bis(benzyloxy)-2-propoxy]methyl chloride (18) to provide the corresponding protected acyclic nucleosides 10a and 19a, which on debenzylation afforded 2,5,6-trichloro-1-[(2-hydroxyethoxy)methyl]benzimidazole (11a) and 2,5,6-trichloro-1-[(1,3-dihydroxy-2-propoxy)methyl] benzimidazole (20a), respectively. A similar condensation of 2,4,6-trichlorobenzimidazole (2a) and 2,4,5-trichlorobenzimidazole (7a) followed by debenzylation yielded 11b, 20b, 11c, and 20c, respectively. A nucleophilic displacement of the 2-chloro group of 11a-c and 20a-c with liquid ammonia, methylamine, dimethylamine, and thiourea furnished several interesting 2-substituted compounds in good yields, e.g., 12-14(a-e), 21-23(a-e), 15-17, and 24-26. Alkylation of the 2-thio analogs 15-17 and 24-26 with benzyl chloride furnished the 2-alkylthio acyclic nucleosides 12d-14d and 21d-23d. Desulfurization of 15 and 24 with Raney Ni furnished 5,6-dichloro-1[(2-hydroxyethoxy)methyl]benzimidazole (12e) and 5,6-dichloro-1-[1,3-dihydroxy-2-propoxy)methyl]benzimidazole (21e), respectively (acyclic analog of 5,6-dichloro-1-beta-D-ribofuranosylbenzimidazole). Similarly the dihalo compounds 13e, 14e, and 23e were prepared in moderate yields from the 2-thio analogs 16,17, and 26. Treatment of 2-bromo-5,6-dichlorobenzimidazole (8b) with 27 and 30 gave the protected acyclic compounds 28a and 31a, which on deacetylation with sodium carbonate and potassium cyanide yielded 2-bromo-5,6-dichloro-1-[(2-hydroxyethoxy)methyl]benzimidazole (29a) and 2-bromo-5,6-dichloro-1-[(1,3-dihydroxy-2-propoxy)methyl]benzimidazole (32a), respectively, in moderate yields. The 2-bromo-4,6-dichlorobenzimidazole and 2-bromo-,5-dichlorbenzimidazole analogs 29b,c and 32b,c were prepared in a similar manner. Compounds were tested for activity against human cytomegalovirus (HCMV) and herpes simplex virus type 1 (HSV-1) and for cytotoxicity. In marked contrast to the ribosylbenzimidazoles, none of the acyclic analogs were specific and potent inhibitors of HCMV. Only the 2-thiobenzyl analogs 12d, 13d, 14d, and 23d and the 2-Br analogs 32a,b were active, but activity was not well separated from cytotoxicity. The lack of specific and potent antiviral activity strongly suggests that these acyclic nucleoside analogs are not phosphorylated by HCMV or HSV-1 gene products and that the ribosylbenzimidazoles do not require phosphorylation for antiviral activity.
TL;DR: A chiral synthesis of pseudosugar synthon (1R,2S,4R,5S)-1-[(benzyloxy)methyl]-2-tert-butyloxy-4-hydroxybicyclo[3.1]hexane (12) is reported in this paper.
Abstract: A new chiral synthesis of the pseudosugar synthon (1R,2S,4R,5S)-1-[(benzyloxy)methyl]-2-tert-butyloxy-4-hydroxybicyclo[3.1.0]hexane (12) is reported. This compound was used as a template for the construction of carbocyclic nucleoside 4, a conformationally rigid analogue of 2′-deoxyaristeromycin. The X-ray structure and 1H NMR analysis confirmed the exclusive North [2′-exo (2E)] conformation of 4 which is vastly different from that of other non-rigid carbocyclic nucleosides. Compound 4 showed good in vitro antiviral activity against human cytomegalovirus and EBV with minimal cytotoxicity. #This manuscript is dedicated to Professor Yoshihisa Mizuno on the occasion of his 75th birthday.
Patent•
18 Oct 1996
TL;DR: The present invention relates to 5-membered heterocycles of the general formula (see fig. I) in which X1 to X5 are as defined in Claim 1, tautomers thereof, stereoisomers thereof including mixtures thereof, and salts thereof, in particular salts thereof with physiologically tolerable acids or bases, which have useful pharmacological properties, preferably aggregation-inhibiting effects, medicaments comprising these compounds, their use and processes for their preparation as discussed by the authors.
Abstract: The present invention relates to 5-membered heterocycles of the general formula (see fig. I) in which X1 to X5 are as defined in Claim 1, tautomers thereof, stereoisomers thereof, including mixtures thereof, and salts thereof, in particular salts thereof with physiologically tolerable acids or bases, which have useful pharmacological properties, preferably aggregation-inhibiting effects, medicaments comprising these compounds, their use and processes for their preparation.
TL;DR: In this article, the 6,5-bicyclic dipeptides (1-aza-5-oxa-2-oxobicyclo[4.3]nonane ring skeletons) were synthesized by a one-step electrochemical cyclization from the di peptides.
Abstract: Novel, highly constrained, 6,5-bicyclic dipeptides (1-aza-5-oxa-2-oxobicyclo[4.3.0]nonane ring skeletons, 2) have been synthesized by a one-step electrochemical cyclization from the dipeptides Boc-(S)-serine-(S)-proline-OMe (Boc-(S)-Ser-(S)-Pro-OMe, 3) and Boc-(R,S)-α-methylserine-(S)-proline-OMe (Boc-(R,S)-α-MeS-(S)-Pro-OMe, 12) in yields of 10−25% and 41%, respectively. The one-pot reaction uses selective anodic amide oxidation to generate an N-acyliminium cation which is trapped by an intramolecular hydroxyl group. The cyclization of Boc-(S)-Ser-(S)-Pro-OMe (3) to the 6,5-bicyclic skeleton 4 was highly diastereoselective, generating a new chiral center with an S configuration. This bicyclic compound was sufficiently stable to trifluoroacetic acid and anhydrous hydrofluoric acid for use in standard solid phase peptide synthesis methodologies. Oxidation of Boc-(R,S)-MeS-(S)-Pro-OMe (12) gave different results for each diastereoisomer. Cyclization only occurred for the S,S-diastereoisomer with very low st...
TL;DR: In this paper, the reaction of Cp2Ti(Me3SiC2SiMe3) with terminal disubstituted α,ω-diynes RC≡C(CH2)nC≡CR affords, after substitution of Me3SiCs2SiME3, bicyclic titanacyclopentadienes via intramolecular cyclization.
TL;DR: In this article, the radiochemical synthesis of (+)-exo-2-(2-[ 18 F]fluoro-5-pyridyl)-7-azabicyclo[2.2.1] heptane was accomplished by Kryptofix® 222 assisted nucleophilic no-carrier-added [ 18 F]-fluorination of (+/-)-exO-2-bromo-5-, 2-Bromo-, 5-Pyride-, 7- methoxycarbonyl -7-Azabicyclecyclo[
Abstract: The radiochemical synthesis of (+/-)-exo-2-(2-[ 18 F]fluoro-5-pyridyl)-7-azabicyclo[2.2.1]heptane ([ 18 F]1) was accomplished by Kryptofix® 222 assisted nucleophilic no-carrier-added [ 18 F]fluorination of (+/-)-exo-2-(2-bromo-5-pyridyl)-7-azabicyclo[2.2.1] heptane (3a). The average radiochemical yield of the final product was 10% and the average specific activity was greater than >2000 mCi/μmol, calculated at end-of-synthesis. The stable fluorine ligand ([ 19 F]1 was prepared by Kryptofix® 222 assisted nucleophilic fluorination of (+/-)-exo-2-(2-bromo-5-pyridyl) - 7- methoxycarbonyl - 7 - azabicyclo[2.2.1]heptane (3b) followed by acid deprotection.
TL;DR: The reaction of (1,2-dimethoxyethane-O,O′)lithium phosphanide with chloro tri-iso-propylsilylphosphane 1 as well as bis(tri-methyl silyl)amide 2 gave single crystals of 2 (monoclinic, P21/c, a = 15105(1), b = 77118(5), c = 20334(1) pm, β = 108972(6)°, Z = 4, wR2 = 00947