Rhodium(II)‐Catalyzed Intramolecular Cycloisomerizations of Methylenecyclopropanes with N‐Sulfonyl 1,2,3‐Triazoles

A novel rhodium(II)‐catalyzed tandem cycloisomerization of methylenecyclopropanes (MCPs) with N‐sulfonyl 1,2,3‐triazoles is disclosed. The reaction produces a series of highly functionalized polycyclic N heterocycles via a rhodium imino carbene intermediate. A distinct feature of this divergent synthesis is that different types of substrates control the reaction pathways. Moreover, several interesting transformations of these products to construct diazabicyclo[3.2.1]octane derivatives are also reported.     

Design and Theoretical Study of Nickel Catalysts for Syndiotactic Polyolefins

A nickel catalyst was nodeled with ligand L^2,[NH=CH-CH=CH-0]^-,which should have potential use as a syndiotactic plyolefin catalyst,and the reaction mechanism was studied by theoretical calculations using the density functinal method at the B3LYP/LANL2MB level.The mechanism involves the formation of the intermediate [NiL^2Me]^ ,in which the metal occupies a T-shaped geometry.This intermediate has two possible structures with the methyl group trans either to the oxygen or to the nitrogen atom of L^2.The results show that both structures can lead to the desired product via similar reaction paths,A and B.Thus,the polymerization could be considered as taking place either with the alkyl group occupying the position trans to the Ni-0 or trans to the Ni-N bond in the catalyst.The polymerization process thus favors the catalysis of syndiotactic polyolefins.The syndiotactic synthesis effects could also be enhanced by varations in the ligand substituents.From energy considerations,we can conclude that it is more favorable for the methyl ttrans-O position to form a complex than to occupy the trans-N position.From bond length considerations,it is also more favoured for ethene to occupy the trans-O position than to occupy the trans-N position.     

Modified Riemschneider Reaction of 3‐Thiocyanatoquinolinediones

The Riemschneider reaction of 3‐thiocyanatoquinoline‐2,4(1H,3H)‐diones with conc. H₂SO₄ was investigated. Using different reaction conditions, 13 types of reaction products were isolated. Compounds bearing a Me, Et, or Bu group at C(3) afforded mainly [1,3]thiazolo[5,4‐c]quinoline‐2,4‐diones and 1,9b‐dihydro‐9b‐hydroxythiazolo[5,4‐c]quinoline‐2,4‐diones. In the case of the 3‐Bu derivatives of the starting compounds, C‐debutylation was also observed. If a Bn group is present at C(3), rapid C‐debenzylation of the starting thiocyanates occurred, yielding [1,3]oxathiolo[4,5‐c]quinoline‐2,4‐diones, and mixtures of mono‐, di‐, and trisulfides derived from 4‐hydroxy‐3‐sulfanylquinoline‐2‐ones. The reaction mechanism of all of the transformations is discussed. All new compounds were characterized by IR, ¹H‐ and ¹³C‐NMR, and EI and ESI mass spectra, and in some cases, ¹⁵N‐NMR spectra were also used to characterize new compounds.     

Visible‐Light‐Induced Trifluoromethylation of Isonitrile‐Substituted Methylenecyclopropanes: Facile Access to 6‐(Trifluoromethyl)‐7,8‐Dihydrobenzo[k]phenanthridine Derivatives

A new visible‐light‐induced trifluoromethylation of isonitrile‐substituted methylenecyclopropanes is developed. A range of substituted 6‐(trifluoromethyl)‐7,8‐dihydrobenzo[k]phenanthridine derivatives are readily furnished by this newly developed tandem reaction with moderate to good yields. This reaction allows the direct formation of two six‐membered rings and three new C?C bonds, including the C?CF₃ bond, under visible light irradiation.     

Synthesis of Some New Benzo[b][1,4]diazepine Based Heterocycles

Preparation of 4‐chloro‐3H‐benzo[b][1,4]diazepine‐2‐carbaldehyde 5 , which is used as a key intermediate in the synthesis of chalcones derivatives, via its condensation with some aromatic acetophenone derivatives under ethanol piperidine condition was described. Also illustrated was the reaction of such chalcones with available nucleophilics and reagents of active methylene group to afford new series of fused and isolated pyrazoles, isoxazolines pyrimidines, pyridines, triazolo[1,5‐a]pyrimidines, benzo[1,4]oxa(thia)zepines, and pyrido[1,2‐a]benzimidazoles incorporating 4‐chloro‐3H‐benzo[b][1,4]diazepine moiety, which have a potential pharmaceutical interest. Furthermore, condensation reaction of 4‐chloro‐3H‐benzo[b][1,4]diazepine‐2‐carbaldehyde with aromatic amine derivatives to afford the Schiff's bases was described. The C═N double bond of the latter compounds has been reacted with chloroketene to give β‐lactams and with sulfanylacetic acid to give the 2‐(4‐oxo‐1,3‐thiazolidinyl)‐substituted derivative. The structures of the newly prepared compounds were established by elemental analysis, IR, MS, and ¹H NMR spectral analysis.     

Synthesis of Some New 2‐Oxo‐N‐[(10H‐phenothiazin‐10‐yl)alkyl] Derivatives of Azetidine‐1‐carboxamides

The synthesis of a new series of 4‐aryl‐3‐chloro‐2‐oxo‐N‐[3‐(10H‐phenothiazin‐10‐yl)propyl]azetidine‐1‐carboxamides, 4a – 4m , is described. Phenothiazine on reaction with Cl(CH₂)₃Br at room temperature gave 10‐(3‐chloropropyl)‐10H‐phenothiazine ( 1 ), and the latter reacted with urea to yield 1‐[3‐(10H‐phenothiazin‐10‐yl)propyl]urea ( 2 ). Further reaction of 2 with several substituted aromatic aldehydes led to N‐(arylmethylidene)‐N′‐[3‐(phenothiazin‐10‐yl)propyl]ureas 3a – 3m , which, on treatment with ClCH₂COCl in the presence of Et₃N, furnished the desired racemic trans‐2‐oxoazetidin‐1‐carboxamide derivatives 4a – 4m . The structures of all new compounds were confirmed by IR, and ¹H‐ and ¹³C‐NMR spectroscopy, FAB mass spectrometry, and chemical methods.     

Kinetics and mechanism of ligand exchange of coordinated cyanide in hexacyanoferrate(II) by nitroso‐R‐salt in the presence of mercury(II) as a catalyst

The kinetics of Hg(II)‐catalyzed reaction between hexacyanoferrate(II) and nitroso‐R‐salt has been followed spectrophotometrically by monitoring the increase in absorbance at 720 nm, the λ_max of green complex, [Fe(CN)₅ N‐R‐salt]^3? as a function of pH, ionic strength, temperature, concentration of reactants, and the catalyst. In this reaction, the coordinated cyanide ion in hexacyanoferrate(II) gets replaced by incoming N‐R‐salt under the following specified reaction conditions: temperature = 25 ± 0.1°C, pH = 6.5 ± 0.2, and I = 0.1 M (KNO₃). The stoichiometry of the complex has been established as 1:1 by mole ratio method. The rate of catalyzed reaction is slow at low pH values and then increases with pH and attains a maximum value between 6.5 and 6.7. The rate finally falls again at higher pH values due to nonavailability of [H⁺] ions needed to regenerate the catalytic species. The rate of reaction increases initially with [N‐R‐salt] and attains a maximum value and then levels off at higher [N‐R‐salt]. The rate of reaction shows a variable order dependence in [Fe(CN)₆^4?] ranging from unity at lower concentration to 0.1 at higher concentrations. The effect of [Hg²⁺] on the reaction rate shows a complex behavior and the same has been explained in detail. The activation parameters for the catalyzed reactions have been evaluated. A most plausible mechanistic scheme has been proposed based on the experimental observations. © 2005 Wiley Periodicals, Inc. Int J Chem Kinet 37: 222–232, 2005     

Four‐Membered Heterometallacyclic d0 and d1 Complexes of Group 4 Metallocenes with Amidato Ligands

A study of the coordination chemistry of different amidato ligands [(R)N?C(Ph)O] (R=Ph, 2,6‐diisopropylphenyl (Dipp)) at Group 4 metallocenes is presented. The heterometallacyclic complexes [Cp₂M(Cl){κ²‐N,O‐(R)N?C(Ph)O}] M=Zr, R=Dipp ( 1 a ), Ph ( 1 b ); M=Hf, R=Ph ( 2 )) were synthesized by reaction of [Cp₂MCl₂] with the corresponding deprotonated amides. Complex 1 a was also prepared by direct deprotonation of the amide with Schwartz reagent [Cp₂Zr(H)Cl]. Salt metathesis reaction of [Cp₂Zr(H)Cl] with deprotonated amide [(Dipp)N?C(Ph)O] gave the zirconocene hydrido complex [Cp₂M(H){κ²‐N,O‐(Dipp)N?C(Ph)O}] ( 3 ). Reaction of 1 a with Mg did not result in the desired Zr(III) complex but in formation of Mg complex [(py)₃Mg(Cl) {κ²‐N,O‐(Dipp)N?C(Ph)O}] ( 4 ; py=pyridine). The paramagnetic complexes [Cp′₂Ti{κ²‐N,O‐(R)N?C(Ph)O}] (Cp′=Cp, R=Ph ( 7 a ); Cp′=Cp, R=Dipp ( 7 b ); Cp′=Cp*, R=Ph ( 8 )) were prepared by the reaction of the known titanocene alkyne complexes [Cp₂′Ti(η²‐Me₃SiC₂SiMe₃)] (Cp′=Cp ( 5 ), Cp′=Cp* ( 6 )) with the corresponding amides. Complexes 1 a , 2 , 3 , 4 , 7 a , 7 b , and 8 were characterized by X‐ray crystallography. The structure and bonding of complexes 7 a and 8 were also characterized by EPR spectroscopy.     

Synthesis,Modification, and Anticonvulsant Activity of 3′‐R1‐Spiro[indoline‐3,6′‐[1,2,4]triazino[2,3‐c]quinazolin]‐2,2′(7′H)‐diones Derivatives

Previously unknown 3′‐R¹‐5‐R²‐spiro[indoline‐3,6′‐[1,2,4]triazino[2,3‐c]quinazoline]‐2,2′‐(7′H)‐diones and their N‐substituted analogues were obtained via reaction of 6‐R¹‐3‐(2‐aminophenyl)‐1,2,4‐triazin‐5‐ones with isatin and its substituted derivatives. It was shown that alkylation of 3′‐R¹‐5‐R²‐spiro[indoline‐3,6′‐[1,2,4]triazino[2,3‐c]quinazolin]‐2,2′‐(7′H)‐diones by N‐R³‐chloroacetamides or chloroacetonitrile in the presence of а base proceeds by N‐1 atom of isatin fragment. The spectral properties (¹H and ¹³C NMR spectra) of synthesized compounds were studied, and features of spectral patterns were discussed. The high‐effective anticonvulsant and radical scavenging agents among 3′‐R¹‐5‐R²‐spiro[indoline‐3,6′‐[1,2,4]triazino[2,3‐c]quinazolin]‐2,2′(7′H)‐diones and their N‐substituted derivatives were detected. It was shown that compounds 2.2 , 2.8 , and 3.1 exceed or compete the activity of the most widely used in modern neurology drug—lamotrigine on the pentylenetetrazole‐induced seizures model. The aforementioned fact may be considered as a reason for further profound study of synthesized compounds using other pathology models.     

Nickel(II)‐Catalyzed Asymmetric Propargyl [2,3] Wittig Rearrangement of Oxindole Derivatives: A Chiral Amplification Effect

A highly enantioselective [2,3] Wittig rearrangement of oxindole derivatives was realized by using a chiral N,N′‐dioxide/Ni^II complex as the catalyst under mild reaction conditions. A strong chiral amplification effect was observed, and allowed access to chiral 3‐hydroxy 3‐substituted oxindoles bearing allenyl groups in high yields and enantioselectivities (up to 92 % ee) by using a ligand with only 15 % ee. A reasonable explanation was given based on the experimental investigations and X‐ray crystal structures of enantiomerically pure and racemic catalysts. Moreover, the first catalytic kinetic resolution of racemic oxindole derivatives by a [2,3] Wittig rearrangement was realized with high efficiency and stereoselectivity.     

Domino Rhodium/Palladium‐Catalyzed Dehydrogenation Reactions of Alcohols to Acids by Hydrogen Transfer to Inactivated Alkenes

The combination of the d⁸ Rh^I diolefin amide [Rh(trop₂N)(PPh₃)] (trop₂N=bis(5‐H‐dibenzo[a,d]cyclohepten‐5‐yl)amide) and a palladium heterogeneous catalyst results in the formation of a superior catalyst system for the dehydrogenative coupling of alcohols. The overall process represents a mild and direct method for the synthesis of aromatic and heteroaromatic carboxylic acids for which inactivated olefins can be used as hydrogen acceptors. Allyl alcohols are also applicable to this coupling reaction and provide the corresponding saturated aliphatic carboxylic acids. This transformation has been found to be very efficient in the presence of silica‐supported palladium nanoparticles. The dehydrogenation of benzyl alcohol by the rhodium amide, [Rh]N, follows the well established mechanism of metal–ligand bifunctional catalysis. The resulting amino hydride complex, [RhH]NH, transfers a H₂ molecule to the Pd nanoparticles, which, in turn, deliver hydrogen to the inactivated alkene. Thus a domino catalytic reaction is developed which promotes the reaction R‐CH₂‐OH+NaOH+2 alkene→R‐COONa+2 alkane.     

Syntheses of thiopyrone and pyrone derivatives by photocyclization reaction of 3‐aryl‐2‐( Benzothien‐3‐yl)propenoic acids

Naphtho[1,2‐b][1]benzothiophene‐6‐carboxylic acids, 6H‐benzo[b]naphtho[2,3‐d]thiopyran‐6‐ones and 6H‐benzo[b]naphtho[2,3‐d]pyran‐6‐ones were synthesized in one step by the photocyclization reaction of 3‐aryl‐2‐([1]benzothien‐3‐yl)propenoic acids. The photocyclization reaction did not occur when the 3‐aryl group contained the electron‐withdrawing nitro group. The assignment of the ¹H and ¹³C nmr spectra of 6H‐benzo[b]naphtho[2,3‐d]thiopyran‐6‐one and 6H‐benzo[b]naphtho[2,3‐d]pyran‐6‐one by two‐dimensional nmr methods is described. The difference between the chemical shift values of H12 for these two compounds is attributed to different molecular geometries.     

C(sp3)H Activation without a Directing Group: Regioselective Synthesis of N‐Ylide or N‐Heterocyclic Carbene Complexes Controlled by the Choice of Metal and Ligand

N‐Ylide complexes of Ir have been generated by C(sp³)?H activation of α‐pyridinium or α‐imidazolium esters in reactions with [Cp*IrCl₂]₂ and NaOAc. These reactions are rare examples of C(sp³)?H activation without a covalent directing group, which—even more unusually—occur α to a carbonyl group. For the reaction of the α‐imidazolium ester [ 3 H]Cl, the site selectivity of C?H activation could be controlled by the choice of metal and ligand: with [Cp*IrCl₂]₂ and NaOAc, C(sp³)?H activation gave the N‐ylide complex 4 ; in contrast, with Ag₂O followed by [Cp*IrCl₂]₂, C(sp²)?H activation gave the N‐heterocyclic carbene complex 5 . DFT calculations revealed that the N‐ylide complex 4 was the kinetic product of an ambiphilic C?H activation. Examination of the computed transition state for the reaction to give 4 indicated that unlike in related reactions, the acetate ligand appears to play the dominant role in C?H bond cleavage.     

Graphical Abstract: HCA 1/2003

The low solubility of pterins can drastically be improved by N²‐acylation or formation of the N²‐[(dimethylamino)methylene] derivatives. Both types of compounds can be alkylated under Mitsunobu conditions to form from N²‐acylpterins (see 2 and 3 ) and their derivatives (see 5, 6, 8, 9, 11, 13, 15 , and 17 ) selectively the O⁴‐alkyl derivatives 22 – 31 , whereas the electron‐donating [(dimethylamino)methyleneamino function in 46 – 51 gives, in a selective reaction, the N(3)‐substitution (→ 52 – 61 ). N²,N²‐Dimethylpterins and 18 and 19 and N²‐methylpterins 20 and 21 direct alkylation also to the O⁴‐position (→ 32 – 35, 38 and 39 ). Deacylation can be achieved under very mild conditions by solvolysis with MeOH ( 22 → 40, 26 → 41 ), and displacement of the O⁴‐[2‐(4‐nitrophenyl)ethyl] group proceeds with ammonia at room temperature to the corresponding pteridin‐2,4‐diamines 42 – 45 . Cleavage of the N²‐[(dimethylamino)methylene] group works well with ammonia (→ 62 – 67 ). The advantage of applying the 2‐(4‐nitrophenyl)ethyl (npe) group as blocking group is seen in its selective removal by 1,8‐diazabicyclo[5.4.0]undec‐7‐ene (DBU) under aprotic conditions without harming the other substituents.     

Pyrrole,methylenpyrroline und iminocyclopentene durch ubergangsmetallkatalysierte codimerisierung von methylencyclopropanen mit keteniminen

(Ph₃P)₄Pd - or (RO)₃P/Ni(COD)₂ - catalysed [3+2]-cycloaddition of methylenecyclopropanes 1a – 1e with the ketenimines 2a, 2b leads selectively to pyrrols, α -methylene- Δ³ -pyrrolines or iminocyclopentenes depending on the substituents of the imino group and the methylenecyclopropanes.     

Estimation of peptide N–Cα bond cleavage efficiency during MALDI‐ISD using a cyclic peptide

Matrix‐assisted laser desorption/ionization in‐source decay (MALDI‐ISD) induces N–C_α bond cleavage via hydrogen transfer from the matrix to the peptide backbone, which produces a c′/z? fragment pair. Subsequently, the z? generates z′ and [z + matrix] fragments via further radical reactions because of the low stability of the z?. In the present study, we investigated MALDI‐ISD of a cyclic peptide. The N–C_α bond cleavage in the cyclic peptide by MALDI‐ISD produced the hydrogen‐abundant peptide radical [M + 2H]⁺? with a radical site on the α‐carbon atom, which then reacted with the matrix to give [M + 3H]⁺ and [M + H + matrix]⁺. For 1,5‐diaminonaphthalene (1,5‐DAN) adducts with z fragments, post‐source decay of [M + H + 1,5‐DAN]⁺ generated from the cyclic peptide showed predominant loss of an amino acid with 1,5‐DAN. Additionally, MALDI‐ISD with Fourier transform‐ion cyclotron resonance mass spectrometry allowed for the detection of both [M + 3H]⁺ and [M + H]⁺ with two ¹³C atoms. These results strongly suggested that [M + 3H]⁺ and [M + H + 1,5‐DAN]⁺ were formed by N–C_α bond cleavage with further radical reactions. As a consequence, the cleavage efficiency of the N–C_α bond during MALDI‐ISD could be estimated by the ratio of the intensity of [M + H]⁺ and [M + 3H]⁺ in the Fourier transform‐ion cyclotron resonance spectrum. Because the reduction efficiency of a matrix for the cyclic peptide cyclo(Arg‐Gly‐Asp‐D‐Phe‐Val) was correlated to its tendency to cleave the N–C_α bond in linear peptides, the present method could allow the evaluation of the efficiency of N–C_α bond cleavage for MALDI matrix development. Copyright © 2016 John Wiley & Sons, Ltd.     

The kinetics and mechanism of the substitution reactions of the aquapentacyanoruthenate(II) ion with naphthalene‐substituted ligands in aqueous medium

The kinetics and mechanism of substitution reaction of [Ru(CN)₅H₂O]^3? anion with two naphthalene‐substituted ligands viz. Lⁿ = nitroso‐R‐salt (NRS) and α‐nitroso‐β‐naphthol (αNβN) have been studied spectrophotometrically by monitoring an increase in absorbance at λ_max = 525 nm corresponding to metal to ligand charge transfer (MLCT) transitions due to formation of substituted [Ru(CN)₅L]^n?3 as a function of pH, ionic strength, temperature, a wide range of ligands concentration, and [Ru(CN)₅H₂O^3?] under pseudo‐first‐order conditions. The experimental observation suggests that [Ru(CN)₅H₂O]^3? ion interacts with both ligands, which finally get converted into corresponding, [Ru(CN)₅L]^n?3 complexes as a final reaction product. The reaction is found to obey first‐order dependence each in [Ru(CN)₅H₂O^3?] and [Lⁿ]. The substituted products, viz. [Ru(CN)₅L]^n?3, in each case have strong MLCT transitions in visible region. The substitutional lability of [Ru(CN)₅H₂O]^3? has been discussed in terms of electronic effect on the M? OH₂ bond interactions. The kinetic observation suggests that the complexation reaction of [Ru(CN)₅H₂O]^3? with both the ligands, i.e., NRS and αNβN, follows an ion pair dissociative mechanism. The thermal activation parameters ΔH^≠ and ΔS^≠ have been calculated using Eyring's equation and provided in support for the proposed mechanistic scheme. © 2010 Wiley Periodicals, Inc. Int J Chem Kinet 43: 21–30, 2011     

Luminescent Study on Nd3+ Complexes Containing Carboxylate‐Dithiolene and Alkoxide‐Dithiolene Ligands

Reaction of ligand L H₂ (4,5‐bis[carboxymethylthio]‐1,3‐dithiol‐2‐thione) with neodymium silyl‐amide (Nd[N(TMS)₂]₃; TMS= ‐SiMe₃), in a ratio 2:1, yields a neodymium‐dithiolene‐carboxylato complex ( 1 ) (Nd( L H) L ). Similarly, reaction of 2 equivalents of L′ H₂ (4,5‐bis[2′‐hydroxyethyl)thio]‐1,3‐dithiol‐2‐thione) and one equivalent of neodymium silyl‐amide (Nd[N(TMS)₂]₃) allowed the isolation of complex 2 , with a ligand:metal ratio of 3:2. ATR‐IR spectrum of 1 displays a broad band characteristic of an OH group showing that one carboxylate group remains protonated. Emission spectrum of complex 1 under excitation in the visible region (at 360 nm i.e. on the ligand) displayed typical emission bands of the Nd³⁺, showing that energy transfer from the ligand to the lanthanide was achieved (i.e. “antenna effect”). No significant quenching from the remaining –OH group was detected. In the case of complex 2 , the main emission bands characteristic of the Nd³⁺ ion have been observed, by excitation at 495 nm.     

Synthesis and crystal structure of novel [1,2,4]oxadiazolo[5,4‐d][1,5]benzothiozepine derivatives containing pyrazole moiety

A series of new substituted‐[1,2,4]oxadiazolo[5,4‐d][1,5]benzothiazepine derivatives containing pyrazole ring 4 / 4′ was synthesized by substituted‐pyrazolo[1,5]benzothiazepines 2 / 2′ and substituted‐benzohydroximinoyl chlorides 3 through the 1,3‐dipolar cycloaddition reaction in the presence of Et₃N at room temperature, and characterized by MS, IR, ¹H NMR and elemental analyses. In addition, the structure of 4′l was determined by X‐ray crystallography. J. Heterocyclic Chem., 2011.     

Synthesis,Structure and Reactivity of PH‐Phosphoraneiminato‐ and Iminophosphoraneiminato Group 4 Transition‐Metal Complexes

The versatile coordination chemistry of the well‐investigated phosphoraneiminato‐ligand R₃PN^— ( I ) was extended by the successive introduction of protons to the phosphorus atom. The position of the resulting equilibrium between the NH‐phosphanylamido‐ [R₂P‐NH^—] and the PH‐phosphoraneiminato‐form [R₂HP=N^—] is affected by the Lewis acidity of the coordinated metal fragment. Experimental studies on complexes with various substitution patterns at the group 4 metal center R₂HP=N[M] ( II ) were unambiguously confirmed by DFT‐calculations. The isolation of group 4 PH‐dihydrido‐phosphoraneiminato‐complexes RH₂P‐N[M] ( III ) is prevented by the low thermodynamic stability of the target molecules, also supported by the results of ab initio calculations. However, an access to the by then unknown transition‐metal substituted iminophosphanes RP=N[M] ( IV ) was verified for the first time. Within extensive studies on the coordination chemistry of bis(imino)phosphoranes RP(=NR′)(=NR″), several species of group 4 complexes R(R′N=)P=N[M] ( V ) were isolated and structurally characterized. In this case, investigations on the NH/PH‐tautomerism were performed exclusively on theoretical level, because the required educts are experimentally non‐accessible due to their kinetic instability.