Efficient synthesis and spectral determination of 11‐[(o‐ m‐ and p‐substituted)‐phenyl]‐8‐chloro‐3,3‐dimethyl‐2,3,4,5,10,11‐hexahydro‐1H‐dibenzo[b,e][1,4]diazepin‐1‐ones

A new synthesis to obtain eleven novel derivatives of 11‐[(o‐ m‐ and p‐substituted)‐phenyl]‐8‐chloro‐3,3‐dimethyl‐2,3,4,5,10,11‐hexahydro‐1H‐dibenzo[b,e][1,4]diazepin‐1‐ones with possible pharmacological activity in the central nervous system in two efficient steps has been developed. The final products were obtained by condensation and cyclization between 3‐[4‐chloro‐1,2‐phenylenediamine]‐5,5‐dimethyl‐2‐cyclohexenone with (o‐ m‐ and p‐substituted)benzaldehyde. The structure of all products was corroborated by ir, ¹H‐nmr, ¹³C‐nmr and high resolution in ms.     

Synthesis and spectral properties of 2‐[(o‐ and p‐substituted)aminophenyl] ‐3H‐5‐[(o‐ and p‐substituted)phenyl]‐7‐chloro‐1,4‐benzodiazepines

A series of twelve new 2‐[(o‐ and p‐substituted)aminophenyl]‐3H‐5‐[(o‐ and p‐substituted)phenyl]‐7‐chloro‐1,4‐benzodiazepines, which have possible pharmacological properties has been obtained. The synthesis was carried out following six steps. The structure of all products was corroborated by ir, ¹H nmr, ¹³C nmr and ms. In addition for the compound 2‐(o‐chloroaminophenyl)‐3H‐5‐(o‐fluorophenyl)‐7‐chloro‐1,4‐benzodiazepine 7, its structure was confirmed by X‐ray diffraction.     

Poly(p‐benzamide) having isopropyl‐substituted chiral tri(ethylene glycol) side Chain: Synthesis and helical conformation

Isopropyl‐substituted tri(ethylene glycol) is used as a chiral side chain of N‐substituted poly(p‐benzamide) in order to increase the difference of stability between the right‐ and left‐handed helical structures of the polymer. The target polymer is synthesized by the chain‐growth condensation polymerization of the corresponding monomer with an initiator using lithium 1,1,1,3,3,3‐hexamethyldisilazide as a base. A circular dichroism (CD) study of the polymer reveals that the CD signal is due to an excess of a thermodynamically controlled right‐handed helical structure of the polymer, and that the replacement of the methyl group with a bulkier isopropyl group at the side chain of poly(p‐benzamide) increases the abundance of right‐handed helical structure in chloroform. © 2015 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2015 , 53, 1623–1628     

Efficient Light‐Induced pKa Modulation Coupled to Base‐Catalyzed Photochromism

Photoswitchable acid–base pairs, whose pK_a values can be reversibly altered, are attractive molecular tools to control chemical and biological processes with light. A significant, light‐induced pK_a change of three units in aqueous medium has been realized for two thermally stable states, which can be interconverted using UV and green light. The light‐induced pK_a modulation is based on incorporating a 3‐H‐thiazol‐2‐one moiety into the framework of a diarylethene photoswitch, which loses the heteroaromatic stabilization of the negatively charged conjugate base upon photochemical ring closure, and hence becomes significantly less acidic. In addition, the efficiency of the photoreactions is drastically increased in the deprotonated state, giving rise to catalytically enhanced photochromism. It appears that protonation has a significant influence on the shape of the ground‐ and excited‐state potential energy surfaces, as indicated by quantum‐chemical calculations.     

Synthesis and spectral properties of 2‐methylthio‐3H‐7‐[(o‐; m‐ and p‐substituted)phenoxy]‐4‐(p‐substituted‐phenyl)‐[1,5]benzodiazepines

A series of eleven new 2‐methylthio‐3H‐7‐[(o‐; m‐ and p‐substituted) phenoxy]‐4‐(p‐substituted‐phenyl)‐[1,5]benzodiazepines, which have potentially useful pharmacological activities, has been synthesized by condensing the 4‐[(o‐; m‐ and p‐R₁)phenoxy]‐1,2‐phenylendiamines with 3,3‐dimercapto‐1‐(p‐R₂‐phenyl)‐2‐propen‐1‐one. Afterward the lH‐[1,5]benzodiazepine‐2‐thiones obtained were treated with sodium hydride and methyl iodide. The structure of all products was corroborated by ir, ¹H nmr, ¹³C nmr and ms.     

Enzyme‐Mediated Preparation of Enantiomerically Pure p‐Menthan‐ 3,9‐diols and Their Use for the Synthesis of Natural p‐Menthane Lactones and Ethers

The diastereoselective preparation of the p‐menthane‐3,9‐diols (±)‐ 12 , (±)‐ 13a , (±)‐ 13b , and (±)‐ 18 and the study of their enzymic resolution is described (Scheme 1). The corresponding enantiomer‐enriched diols obtained by means of the lipase‐mediated kinetic acetylation of the racemic diols are suitable synthetic precursors of many relevant p‐menthane monoterpenes. Their usefulness is shown in the preparation of different natural products of this class that are interesting for industrial purposes because of their odor qualities, i.e., of the enantiomeric form of 3‐hydroxy‐p‐menthan‐9‐oic acid lactone 1 , of mintlactone 2 , of the 3,9‐epoxy‐p‐menth‐1,8(10)‐diene 10 , and of the pheromone vesperal 11 (Schemes 2 and 3).     

1,8‐Diazabicyclo[5.4.0]undec‐7‐ene: A Remarkable Base in the Debromination of 4‐ or 5‐Substituted N‐Benzyl α‐Bromo‐α‐p‐Toluenesulfonylglutarimide

Debromination of N‐benzyl 4‐ or 5‐substituted α‐bromo‐α‐p‐toluenesulfonylglutarimides is achieved with 1,8‐diazabicyclo[5.4.0]undec‐7‐ene (DBU) to give the N‐benzyl 4‐ or 5‐substituted α‐p‐toluenesulfonylglutarimides. The DBU/THF system is applied to a new methodology for the synthesis of bicyclic glutarimide skeleton in moderate yields.     

Synthesis and Thermal Properties of Regio‐ and Stereoregular Poly(silylene‐1,4‐phenylenevinylene)s

Polymerization of p‐(dimethylsilyl)phenylacetylene in toluene at 25 and 80°C using RhI(PPh₃)₃ as the catalyst afforded highly regio‐ and stereoregular poly(dimethylsilylene‐1,4‐phenylenevinylene)s (cis‐ 3 a and trans‐ 3 a ) containing 98% cis‐ and 99% trans‐vinylene moieties, respectively. Similarly, poly(butylmethylsilylene‐1,4‐phenylenevinylene)s ( 3 b with 91% cis‐ and 95% trans‐structures) and poly(diisopropylsilylene‐1,4‐phenylenevinylene) with 95% trans‐structure were synthesized. All polymers were soluble in common organic solvents. The trans‐type polymers showed red shifts and hyperchromic effects in the UV‐visible spectrum. The onset temperature of weight loss (T₀) of cis‐ 3 a was much higher than that of trans‐ 3 a .     

A Metal–Organic Framework Containing Unusual Eight‐Connected Zr–Oxo Secondary Building Units and Orthogonal Carboxylic Acids for Ultra‐sensitive Metal Detection

Two metal–organic frameworks (MOFs) with Zr–oxo secondary building units (SBUs) were prepared by using p,p′‐terphenyldicarboxylate (TPDC) bridging ligands pre‐functionalized with orthogonal succinic acid (MOF‐ 1 ) and maleic acid groups (MOF‐ 2 ). Single‐crystal X‐ray structure analysis of MOF‐ 1 provides the first direct evidence for eight‐connected SBUs in UiO‐type MOFs. In contrast, MOF‐ 2 contains twelve‐connected SBUs as seen in the traditional UiO MOF topology. These structural assignments were confirmed by extended X‐ray absorption fine structure (EXAFS) analysis. The highly porous MOF‐ 1 is an excellent fluorescence sensor for metal ions with the detection limit of <0.5 ppb for Mn²⁺and three to four orders of magnitude greater sensitivity for metal ions than previously reported luminescent MOFs.     

Conformational Flexibility and Dynamics of Two (1→6)‐Linked Disaccharides Related to an Oligosaccharide Epitope Expressed on Malignant Tumour Cells

The conformational flexibility and dynamics of two (1→6)‐linked disaccharides that are related to the action of the glycosyl transferase GnT‐V have been investigated. NMR NOE and T‐ROE spectroscopy experiments, conformation‐dependent coupling constants and molecular dynamics (MD) simulations were used in the analyses. To facilitate these studies, the compounds were synthesised as α‐d‐ [6‐¹³C]‐Manp‐OMe derivatives, which reduced the ¹H NMR spectral overlap and facilitated the determination of two‐ and three‐bond ¹H,¹H, ¹H,¹³C and ¹³C,¹³C‐coupling constants. The population distribution for the glycosidic ω torsion angle in α‐d‐ Manp‐(1→6)‐α‐d‐ Manp‐OMe for gt/gg/tg was equal to 45:50:5, whereas in α‐d‐ Manp‐OMe it was determined to be 56:36:8. The dynamic model that was generated for β‐d‐ GlcpNAc‐(1→6)‐α‐d‐ Manp‐OMe by MD simulations employing the PARM22/SU01 CHARMM‐based force field was in very good agreement with experimental observations. β‐d‐ GlcpNAc‐(1→6)‐α‐d‐ Manp‐OMe is described by an equilibrium of populated states in which the ? torsion angle has the exo‐anomeric conformation, the ψ torsion angle an extended antiperiplanar conformation and the ω torsion angle a distribution of populations predominantly between the gauche–trans and the gauche–gauche conformational states (i.e., gt/gg/tg) is equal to 60:35:5, respectively. The use of site‐specific ¹³C labelling in these disaccharides leads to increased spectral dispersion, thereby making NMR spectroscopy based conformational analysis possible that otherwise might be difficult to attain.     

Preparation of C2‐Symmetric Bis[2‐(diphenylphosphino)ferrocen‐1‐yl]‐ methane and Its Use in Rhodium‐ and Ruthenium‐Catalyzed Hydrogenation

The two diphosphine ligands (R_p,R_p)‐ and (S_p,S_p)‐bis[2‐(diphenylphospino)ferrocenyl]methane, (R_p,R_p)‐ and (S_p,S_p)‐ 1 , resp., were prepared in six steps from (S)‐ and (R)‐ferrocenyl tolyl sulfoxide, respectively (Scheme). In the solid state, both the diborane complex (R_p,R_p)‐ 1 ? (BH₃)₂ and the palladium dichloride complex [PdCl₂((R_p,R_p)‐ 1 )] were found to adopt C₂‐pseudosymmetric structures according to X‐ray analyses (Figs. 2 and 3). In the Rh‐ and Ru‐catalyzed hydrogenation of selected alkenes and ketones in the presence of the new ligands, enantioselectivities of up to 55% ee were obtained.     

Synthesis of poly(p‐methoxyphenylacetylene) with the vanadium acetylacetonate‐aluminum triethyl Ziegler–Natta catalyst system: Cyclotrimers/polymer ratio analysis

Poly(p‐methoxyphenylacetylene) was obtained by the reaction of p‐methoxyphenylacetylene (MOPA) with the vanadium acetylacetonate‐aluminum triethyl V(acac)₃‐AlEt₃ homogeneous catalyst system. The crude product was always a mixture of 1,2,4‐ and 1,3,5‐tris(p‐methoxyphenyl)benzene and poly(MOPA) of low averaged molecular weight. The 1,2,4‐ and 1,3,5‐cyclotrimers versus poly(MOPA) ratio was analyzed. The poly(MOPA) obtained under different conditions, on the basis of the spectroscopic data, always shows a cis–transoidal stereo‐regular structure. Molecular mass of poly(MOPA) was determined by vapor pressure osmometry, high pressure liquid chromatography (HPLC), and gel permeation chromatography (GPC) techniques. The kinetics of the reaction has been also analyzed. © 2005 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 43: 5987–5997, 2005     

Kinetics of elimination reactions of 1,2‐diphenyl ethyl substrates in acetonitrile: A mechanistic change in the presence of a strong base

Kinetics of elimination of methanesulfonic acid from 1,2‐diphenylethylmethane sulfonate and its 1‐p‐methylphenyl‐ and 1‐p‐chlorophenyl‐substituted derivatives is studied. The results show that the elimination reaction is unimolecular (E1) as reported in the case of 1‐chloro‐1‐(4‐methoxyphenyl)‐2‐phenylethane. The rate of the elimination reaction in the presence of added weak base pyridine is independent of the concentration of the base, but in the presence of a strong base piperidine the rate shows a linear upward drift and this is due to the appearance of a bimolecular component along with the unimolecular pathway. The shift from the unimolecular to bimolecular process takes place independently of the nature of the leaving group and the parasubstituent in the 1,2‐diphenylethyl substrate. © 2008 Wiley Periodicals, Inc. 40: 481–487, 2008     

δ‐Peptide Analogues of Pyranosyl‐RNA,Part 1 , Nucleo‐δ‐peptides Derived from Conformationally Constrained Nucleo‐δ‐amino Acids: Preparation of Monomers

Cyclic nucleo‐δ‐amino acids that constitute monomers of a conformationally constrained nucleo‐δ‐peptide base‐pairing system have been prepared. Their synthesis starts with an enantioselectively catalyzed chirogenic Diels‐Alder reaction, proceeds via a regioselective ε‐iodolactamization process, and ends with a regio‐ as well as diastereoselective introduction of nucleobases through S_N2‐type opening of a transiently formed N‐acylaziridine ring. Extensive use of X‐ray crystal‐structure analysis has been made to support structure assignments.     

Photocontrol of the Catalytic Activity of a β‐Cyclodextrin Bearing Azobenzene and Histidine Moieties as a Pendant Group

An azobenzene group was linked to β‐cyclodextrin via a histidine spacer ( 1 ) to produce a photoresponsive catalyst. The ester hydrolysis of p‐nitrophenyl acetate, Boc‐L ‐alanine‐p‐nitrophenyl ester and Boc‐D ‐alanine‐p‐nitrophenyl ester was examined in the presence of trans‐ 1 or cis‐ 1 . In the case of cis‐ 1 , the cyclodextrin cavity was used as the substrate binding site during imidazole‐catalyzed ester hydrolysis. This was not possible in the case of trans‐ 1 due to the inclusion of the trans‐azobenzene moiety in the cyclodextrin cavity. Consequently, the catalytic mechanism switches in an on‐off fashion on UV irradiation, associated with the conversion of the azobenzene moiety of 1 from trans to cis.     

Reactions of Methyl Diazoacetate with (E)‐ and (Z)‐1,2‐Bis(trifluoromethyl)ethene‐1,2‐dicarbonitrile: Novel and Unanticipated Pathways

The cycloadditions of methyl diazoacetate to 2,3‐bis(trifluoromethyl)fumaronitrile ((E)‐ BTE ) and 2,3‐bis(trifluoromethyl)maleonitrile ((Z)‐ BTE ) furnish the 4,5‐dihydro‐1H‐pyrazoles 13 . The retention of dipolarophile configuration proceeds for (E)‐ BTE with > 99.93% and for (Z)‐ BTE with > 99.8% (CDCl₃, 25°), suggesting concertedness. Base catalysis (1,4‐diazabicyclo[2.2.2]octane (DABCO), proton sponge) converts the cycloadducts, trans‐ 13 and cis‐ 13 , to a 94 : 6 equilibrium mixture (CDCl₃, r.t.); the first step is N‐deprotonation, since reaction with methyl fluorosulfonate affords the 4,5‐dihydro‐1‐methyl‐1H‐pyrazoles. Competing with the cis/trans isomerization of 13 is the formation of a bis(dehydrofluoro) dimer (two diastereoisomers), the structure of which was elucidated by IR, ¹⁹F‐NMR, and ¹³C‐NMR spectroscopy. The reaction slows when DABCO is bound by HF, but F^? as base keeps the conversion to 22 going and binds HF. The diazo group in 22 suggests a common intermediate for cis/trans isomerization of 13 and conversion to 22 : reversible ring opening of N‐deprotonated 13 provides 18 , a derivative of methyl diazoacetate with a carbanionic substituent. Mechanistic comparison with the reaction of diazomethane and dimethyl 2,3‐dicyanofumarate, a related tetra‐acceptor‐ethylene, brings to light unanticipated divergencies.     

Synthesis and Absolute Configuration at C(8) of ‘p‐Menthane‐3,8,9‐triol’ Derived from (–)‐Isopulegol

Two diastereoisomers of the new, potentially insecticidal ‘p‐menthane‐3,8,9‐triol’ (=(2S)‐ and (2R)‐ 2‐[(1R,2R,4R)‐2‐hydroxy‐4‐methylcyclohexyl]propane‐1,2‐diol; (8S)‐ and (8R)‐ 1 ), have been synthesized from (–)‐isopulegol by both conventional dihydroxylation and catalytic Sharpless dihydroxylation (Scheme). The absolute configuration at C(8) of the corresponding orthoformate adduct (8S)‐ 3a was determined by ¹H‐NMR and X‐ray crystallographic analysis (Figure).     

Enzyme‐Mediated Preparation of (+)‐ and (−)‐β‐Irone and (+)‐ and (−)‐cis‐γ‐Irone from Irone alpha®

The (−)‐ and (+)‐β‐irones ((−)‐ and (+)‐ 2 , resp.), contaminated with ca. 7 – 9% of the (+)‐ and (−)‐trans‐α‐isomer, respectively, were obtained from racemic α‐irone via the 2,6‐trans‐epoxide (±)‐ 4 (Scheme 2). Relevant steps in the sequence were the LiAlH₄ reduction of the latter, to provide the diastereoisomeric‐4,5‐dihydro‐5‐hydroxy‐trans‐α‐irols (±)‐ 6 and (±)‐ 7 , resolved into the enantiomers by lipase‐PS‐mediated acetylation with vinyl acetate. The enantiomerically pure allylic acetate esters (+)‐ and (−)‐ 8 and (+)‐ and (−)‐ 9 , upon treatment with POCl₃/pyridine, were converted to the β‐irol acetate derivatives (+)‐ and (−)‐ 10 , and (+)‐ and (−)‐ 11 , respectively, eventually providing the desired ketones (+)‐ and (−)‐ 2 by base hydrolysis and MnO₂ oxidation. The 2,6‐cis‐epoxide (±)‐ 5 provided the 4,5‐dihydro‐4‐hydroxy‐cis‐α‐irols (±)‐ 13 and (±)‐ 14 in a 3 : 1 mixture with the isomeric 5‐hydroxy derivatives (±)‐ 15 and (±)‐ 16 on hydride treatment (Scheme 1). The POCl₃/pyridine treatment of the enantiomerically pure allylic acetate esters, obtained by enzymic resolution of (±)‐ 13 and (±)‐ 14 , provided enantiomerically pure cis‐α‐irol acetate esters, from which ketones (+)‐ and (−)‐ 22 were prepared (Scheme 4). The same materials were obtained from the (9S) alcohols (+)‐ 13 and (−)‐ 14 , treated first with MnO₂, then with POCl₃/pyridine (Scheme 4). Conversely, the dehydration with POCl₃/pyridine of the enantiomerically pure 2,6‐cis‐5‐hydroxy derivatives obtained from (±)‐ 15 and (±)‐ 16 gave rise to a mixture in which the γ‐irol acetates 25a and 25b and 26a and 26b prevailed over the α‐ and β‐isomers (Scheme 5). The (+)‐ and (−)‐cis‐γ‐irones ((+)‐ and (−)‐ 3 , resp.) were obtained from the latter mixture by a sequence involving as the key step the photochemical isomerization of the α‐double bond to the γ‐double bond. External panel olfactory evaluation assigned to (+)‐β‐irone ((+)‐ 2 ) and to (−)‐cis‐γ‐irone ((−)‐ 3 ) the strongest character and the possibility to be used as dry‐down note.     

Two‐Photon Absorption Cross‐Sections of Reference Dyes: A Critical Examination

The electronic structure and one‐ and two‐photon absorption spectra of four fluorophores, p‐bis(o‐methoxystyryl)benzene (Bis‐MSB), coumarin 307, fluorescein and rhodamine B, commonly used as reference compounds for two‐photon absorption spectra, have been theoretically calculated and compared with available experimental data. The possible reasons for the wide discrepancies in two‐photon absorption cross‐sections reported in the literature are discussed on the basis of the theoretical findings. The role of a solvent environment on the electronic one‐ and two‐photon absorption spectra is also studied. We highlight some necessary precautions that one needs to take when comparing literature results of two‐photon absorption cross‐sections.     

New Types of Planar Chiral [2.2]Paracyclophanes and Construction of One‐Handed Double Helices

New types of planar chiral (R_p)‐ and (S_p)‐4,7,12,15‐tetrasubstituted [2.2]paracyclophanes were synthesized from racemic 4,12‐dihydroxy[2.2]paracyclophane as the starting compound. Regioselective dibromination and transformation afforded a series of planar chiral (R_p)‐ and (S_p)‐4,7,12,15‐tetrasubstituted [2.2]paracyclophanes, which can be used as chiral building blocks. In this study, left‐ and right‐handed double helical structures were constructed via chemoselective Sonogashira–Hagihara coupling. The double helical compounds were excellent circularly polarized luminescence (CPL) emitters with large molar extinction coefficients, good photoluminescence quantum efficiencies, and large CPL dissymmetry factors.