Hierarchical Superstructures with Control of Helicity from the Self‐Assembly of Chiral Bent‐Core Molecules

Herein, two asymmetric chiral bent‐core molecules, 3‐[(4‐{[4‐(heptyloxy)benzoyl]oxy}benzoyl)oxy]‐phenyl‐4‐[(4‐{[(1R)‐1‐methylheptyl]oxy}benzoyl)oxy] benzoate (BC7R) and 3‐[(4‐{[4‐(heptyloxy)benzoyl]oxy}benzoyl)oxy]‐phenyl‐4‐[(4‐{[(1S)‐1‐methylheptyl]oxy}benzoyl)oxy] benzoate (BC7S), were synthesized to demonstrate control of the helicity of their self‐assembled hierarchical superstructures. Mirror‐imaged CD spectra showed a split‐type Cotton effect after the formation of self‐assembled aggregates of BC7R and BC7S, thereby suggesting the formation of intermolecular exciton couplets with opposite optical activities. Both twisted and helical ribbons with preferential helicity that corresponded to the twisting character of the intermolecular exciton couplet were found in the aggregates. The formation of helical ribbons was attributed to the merging of twisted ribbons through an increase in width to improve morphological stability. As a result, control of the helicity of hierarchical superstructures from the self‐assembly of bent‐core molecules could be achieved by taking advantage of the transfer of chiral information from the molecular level onto the hierarchical scale.     

Concise Synthesis of [1,1′‐Biisoquinoline]‐4,4′‐diol via a Protecting Group Strategy and Its Application for Potential Liquid‐Crystalline Compounds

The [1,1′‐biisoquinoline]‐4,4′‐diol ( 4a ), which was obtained as hydrochloride 4a ?2 HCl in two steps starting from the methoxymethyl (MOM)‐protected 1‐chloroisoquinoline 8 (Scheme 3), opens access to further O‐functionalized biisoquinoline derivatives. Compound 4a ?2 HCl was esterified with 4‐(hexadecyloxy)benzoyl chloride ( 5b ) to give the corresponding diester 3b (Scheme 4), which could not be obtained by Ni‐mediated homocoupling of 6b (Scheme 2). The ether derivative 2b was accessible in good yield by reaction of 4a ?2 HCl with the respective alkyl bromide 9 under the conditions of Williamson etherification (Scheme 4). Slightly modified conditions were applied to the esterification of 4a ?2 HCl with galloyl chlorides 10a – h as well as etherification of 4a ?2 HCl with 6‐bromohexyl tris(alkyloxy)benzoates 11b , d – h and [(6‐bromohexyl)oxy]‐substituted pentakis(alkyloxy)triphenylenes 14a – c (Scheme 5). Despite the bulky substituents, the respective target 1,1′‐biisoquinolines 12, 13 , and 15 were isolated in 14–86% yield (Table).     

Eudesmane‐Type Sesquiterpene Derivatives from Saussurea conica

Four new eudesmane‐type sesquiterpene derivatives, 3β‐[(β‐D ‐glucopyranosyl)oxy]‐11αH‐eudesm‐4(14)‐en‐12,8β‐olide ( 1 ), (3β)‐eudesma‐4(14),11(13)‐diene‐3,12‐diol ( 2 ), 3β‐[(β‐D ‐glucopyranosyl)oxy]eudesma‐4(14),11(13)‐dien‐12‐ol ( 3 ), and 3β‐[(β‐D ‐glucopyranosyl)oxy]eudesm‐4(14)‐en‐11‐ol ( 4 ), together with the known (3β)‐eudesm‐4(14)‐ene‐3,11‐diol ( 5 ) were isolated from Saussurea conica, and their structures were elucidated both spectroscopically and by chemical methods.     

3‐Rhoda‐1,2‐diazacyclopentanes: A Series of Novel Metallacycle Complexes Derived From CN Functionalization of Ethylene

Rh‐containing metallacycles, [(TPA)Rh^III(κ²‐(C,N)‐CH₂CH₂(NR)₂‐]Cl; TPA=N,N,N,N‐tris(2‐pyridylmethyl)amine have been accessed through treatment of the Rh^I ethylene complex, [(TPA)Rh(η²‐CH₂CH₂)]Cl ([ 1 ]Cl) with substituted diazenes. We show this methodology to be tolerant of electron‐deficient azo compounds including azo diesters (RCO₂N?NCO₂R; R=Et [ 3 ]Cl, R=iPr [ 4 ]Cl, R=tBu [ 5 ]Cl, and R=Bn [ 6 ]Cl) and a cyclic azo diamide: 4‐phenyl‐1,2,4‐triazole‐3,5‐dione (PTAD), [ 7 ]Cl. The latter complex features two ortho‐fused ring systems and constitutes the first 3‐rhoda‐1,2‐diazabicyclo[3.3.0]octane. Preliminary evidence suggests that these complexes result from N–N coordination followed by insertion of ethylene into a [Rh]?N bond. In terms of reactivity, [ 3 ]Cl and [ 4 ]Cl successfully undergo ring‐opening using p‐toluenesulfonic acid, affording the Rh chlorides, [(TPA)Rh^III(Cl)(κ¹‐(C)‐CH₂CH₂(NCO₂R)(NHCO₂R)]OTs; [ 13 ]OTs and [ 14 ]OTs. Deprotection of [ 5 ]Cl using trifluoroacetic acid was also found to give an ethyl substituted, end‐on coordinated diazene [(TPA)Rh^III(κ²‐(C,N)‐CH₂CH₂(NH)₂‐]⁺ [ 16 ]Cl, a hitherto unreported motif. Treatment of [ 16 ]Cl with acetyl chloride resulted in the bisacetylated adduct [(TPA)Rh^III(κ²‐(C,N)‐CH₂CH₂(NAc)₂‐]⁺, [ 17 ]Cl. Treatment of [ 1 ]Cl with AcN?NAc did not give the Rh?N insertion product, but instead the N,O‐chelated complex [(TPA)Rh^I ( κ²‐(O,N)‐CH₃(CO)(NH)(N?C(CH₃)(OCH?CH₂))]Cl [ 23 ]Cl, presumably through insertion of ethylene into a [Rh]?O bond.     

New Methods for the Synthesis of 3‐Amino‐6,7‐Dihydro‐5H‐Cyclopenta[c]Pyridine‐4‐Carbonitriles and Cyclopenta[d]Pyrazolo[3,4‐b]Pyridines via a Smiles‐type Rearrangement

By reaction with sodium ethoxide and as a function of their structures, 2‐[(1‐alkyl(aryl)‐4‐cyano‐6,7‐dihydro‐5H‐cyclopenta[c ]pyridin‐3‐yl)oxy]acetamides 11 gave 1‐amino‐5‐alkyl(aryl)‐7,8‐dihydro‐6H‐cyclopenta[d ]furo[2,3‐b ]pyridine‐2‐carboxamides 10 and/or 1‐alkyl(aryl)‐3‐amino‐6,7‐dihydro‐5H‐cyclopenta[c ]pyridine‐4‐carbonitriles 12 .     

Efficient Synthesis of 1‐Aryl‐4‐[(ethoxycarbonyl)oxy]‐1H‐pyrazole‐3‐carboxylates

Two‐step synthesis of N‐aryl 4‐[(ethoxycarbonyl) oxy]‐1H‐pyrazole‐3‐carboxylates is achieved starting from the commercially available ethyl 4‐chloroacetoacetate and aromatic amines. Azo coupling followed by cyclization with ethyl chloroformate–DMAP pair resulted in the formation of new 4‐oxy‐1H‐pyrazole derivatives in high yields.     

Nitrene Insertion into CC and CH Bonds of Diamide Diimine Ligands Ligated to Chromium and Iron

The impact of redox non‐innocence (RNI) on chemical reactivity is a forefront theme in coordination chemistry. A diamide diimine ligand, [{‐CH?N(1,2‐C₆H₄)NH(2,6‐iPr₂C₆H₃)}₂]ⁿ (n=0 to ?4), (dadi)ⁿ, chelates Cr and Fe to give [(dadi)M] ([ 1 Cr(thf)] and [ 1 Fe]). Calculations show [ 1 Cr(thf)] (and [ 1 Cr]) to have a d⁴ Cr configuration antiferromagnetically coupled to (dadi)^2?*, and [ 1 Fe] to be S=2. Treatment with RN₃ provides products where RN is formally inserted into the C? C bond of the diimine or into a C? H bond of the diimine. Calculations on the process support a mechanism in which a transient imide (imidyl) aziridinates the diimine, which subsequently ring opens.     

Activation of Homolytic SiZn and SiHg Bond Cleavage,Mediated by a Pt0 Complex,via Novel PtZn and PtHg Compounds

The thermally stable [(tBuMe₂Si)₂M] (M=Zn, Hg) generate R₃Si^. radicals in the presence of [(dmpe)Pt(PEt₃)₂] at 60–80 °C. The reaction proceeds via hexacoordinate Pt complexes, (M=Zn ( 2 a and 2 b ), M=Hg ( 3 a and 3 b )) which were isolated and characterized. Mild warming or photolysis of 2 or 3 lead to homolytic dissociation of the Pt? MSiR₃ bond generating silyl radicals and novel unstable pentacoordinate platinum paramagnetic complexes (M=Zn ( 5 ), Hg ( 6 )) whose structures were determined by EPR spectroscopy and DFT calculations.     

Steroidal Saponins from Disporopsis pernyi

Four new steroidal saponins, named disporosides A–D ( 1 – 4 ), corresponding to (3β,25R)‐3‐[(β‐D ‐glucopyranosyl‐(1→2)‐[β‐D ‐glucopyranosyl‐(1→6)]‐β‐D ‐glucopyranosyl)oxy]‐5β‐spirostan ( 1 ), (3β,25R)‐3‐[(β‐D ‐glucopyranosyl‐(1→2)‐[6‐O‐hexadecanoyl‐β‐D ‐glucopyranosyl‐(1→6)]‐β‐D ‐glucopyranosyl)oxy]‐5β‐spirostan ( 2 ), (3β,22R,25R)‐26‐[(β‐D ‐glucopyranosyl)oxy]‐3‐[(β‐D ‐glucopyranosyl‐(1→2)‐β‐D ‐glucopyranosyl)oxy]‐5β‐furostan ( 3 ), and (3β,22R,25R)‐26‐[(β‐D ‐glucopyranosyl)oxy]‐3‐[(β‐D ‐glucopyranosyl‐(1→2)‐[β‐D ‐glucopyranosyl‐(1→6)]‐β‐D ‐glucopyranosyl)oxy]‐5β‐furostan ( 4 ), have been isolated from the fresh rhizomes of Disporopsis pernyi, together with the three known compounds Ys‐I, agavoside B, and (3β,25R)‐3‐[(β‐D ‐xylopyranosyl‐(1→3)‐β‐D ‐glucopyranosyl‐(1→4)‐β‐D ‐galactopyranosyl)oxy]‐5α‐spirostan‐12‐one. Their structures were elucidated by spectroscopic analyses, chemical transformations (acid hydrolysis), and comparison with literature data.     

Phenolic Derivatives from the Root Bark of Oplopanax horridus

Four new phenolic derivatives, including two phenylpropanoid glycosides, one benzoate glycoside, and one lignan glycoside, together with one known glyceride, were isolated from the root bark of Oplopanax horridus. The structures of the new compounds were elucidated as 3‐{4‐[(6‐O‐acetyl‐β‐D ‐glucopyranosyl)oxy]‐3,5‐dimethoxyphenyl}propanoic acid ( 1 ), (+)‐[5,6,7,8‐tetrahydro‐7‐(hydroxymethyl)‐10,11‐dimehoxydibenzo[a,c][8]annulen‐6‐yl]methyl β‐D ‐glucopyranoside ( 2 ), (+)‐methyl 4‐[6‐O‐{3‐hydroxy‐3‐methyl‐5‐(1‐methylpropyl)oxy]‐5‐oxopentanoyl}‐4‐O‐(β‐D ‐glucopyranosyl)‐β‐D ‐glucopyranosyl)oxy]‐3‐methoxybenzoate ( 3 ), and 2‐methoxy‐4‐[(1E)‐3‐methoxy‐3‐oxoprop‐1‐en‐1‐yl]phenyl 6‐O‐{3‐hydroxy‐3‐methyl‐5‐[(1‐methylpropyl)oxy]‐5‐oxopentanoyl‐4‐O‐β‐d‐ glucopyranosyl‐β‐d‐ glucopyranoside ( 4 ) on the basis of spectroscopic techniques including NMR and MS analyses. The known compound was identified as glycer‐2‐yl ferulate ( 5 ) by comparing its physical and spectral data with those reported in the literature.     

Soluble Polystyrenes Functionalized by Triorgano[(1‐oxoalkyl)oxy]stannanes (=Triorganotin Carboxylates): Synthesis,Structure, and Anion‐Recognition Characteristics

Polystyrene copolymers of the type ( P −H)_1−x( P −(CH₂)_n−COOSnR₃)_x containing [(1‐oxoalkyl)oxy]triphenylstannane or tributyl[(1‐oxoalkyl)oxy]stannanes as side chains ( P −H=styrene; P −(CH₂)_n−COOSnR₃ =para‐substituted styrene‐like monomeric unit with R=Ph (x=0.1), Bu (x=0.5); n=2–4) were investigated. The tributyl[(1‐oxoalkyl)oxy]stannane copolymer was prepared by direct conversion of the corresponding copolymeric methyl esters with hexabutyldistannoxane. By contrast, the [(1‐oxoalkyl)oxy]triphenylstannane copolymer could be prepared only by a procedure involving two reaction steps consisting of a preliminary hydrolysis of the related methyl ester ( P −H)_1‐x( P −(CH₂)_n−COOMe)_x followed by functionalization of the corresponding poly(carboxylic acid) ( P −H)_1‐x( P −(CH_2n−COOH)_x with hydroxytriphenylstannane. Attempts to directly convert the methyl ester with hydroxytriphenylstannane or hexaphenyldistannoxane led to the formation of uncompletely functionalized product. The structure of the stannane‐functionalized polymers was investigated in solution and solid state by NMR, IR, and thermal analysis. The tributylstannane and triphenylstannane copolymers were assessed as chloride‐selective anion carriers in polymeric‐liquid‐membrane potentiometric ion‐selective electrodes.     

Understanding the Mechanisms of Unusually Fast HH,CH,and CC Bond Reductive Eliminations from Gold(III) Complexes

Carbon–carbon bond reductive elimination from gold(III) complexes are known to be very slow and require high temperatures. Recently, Toste and co‐workers have demonstrated extremely rapid C?C reductive elimination from cis‐[AuPPh₃(4‐F‐C₆H₄)₂Cl] even at low temperatures. We have performed DFT calculations to understand the mechanistic pathway for these novel reductive elimination reactions. Direct dynamics calculations inclusive of quantum mechanical tunneling showed significant contribution of heavy‐atom tunneling (>25 %) at the experimental reaction temperatures. In the absence of any competing side reactions, such as phosphine exchange/dissociation, the complex cis‐[Au(PPh₃)₂(4‐F‐C₆H₄)₂]⁺ was shown to undergo ultrafast reductive elimination. Calculations also revealed very facile, concerted mechanisms for H?H, C?H, and C?C bond reductive elimination from a range of neutral and cationic gold(III) centers, except for the coupling of sp³ carbon atoms. Metal–carbon bond strengths in the transition states that originate from attractive orbital interactions control the feasibility of a concerted reductive elimination mechanism. Calculations for the formation of methane from complex cis‐[AuPPh₃(H)CH₃]⁺ predict that at ?52 °C, about 82 % of the reaction occurs by hydrogen‐atom tunneling. Tunneling leads to subtle effects on the reaction rates, such as large primary kinetic isotope effects (KIE) and a strong violation of the rule of the geometric mean of the primary and secondary KIEs.     

Deprotonation of Coordinated Phosphanes in a Rhenium Complex: CC Coupling with Diimine Coligands

The reaction of fac‐[Re(bipy)(CO)₃(PMe₃)][OTf] (bipy=2,2′‐bipyridine) with KN(SiMe₃)₂ affords two neutral products: cis,trans‐[Re(bipy)(CO)₂(CN)(PMe₃)], and a thermally unstable compound, which features a new C?C bond between a P‐bonded methylene group (from methyl group deprotonation) and the C6 position of bipy. The solid‐state structures of more stable 1,2‐bis[(2,6‐diisopropylphenyl)imino]acenaphthene analogs, resulting from the deprotonation of PMe₃, PPhMe₂, and PPh₂Me ligands, are determined by X‐ray diffraction.     

Asymmetric Mannich‐Type Synthesis of N‐Phosphinyl α‐Aminophosphonic Acid Monoesters

A convenient diastereoselective synthesis of diisopropyl (2R,3R)‐3‐{{{(R/S)‐aryl[(diethoxyphosphinyl)amino]methyl}hydroxyphosphinyl}oxy}‐2‐hydroxybutanedioate through Mannich‐type reactions is reported. The reactions take place under mild conditions in good yields, and this makes it possible to introduce various substituents at the α‐position to the P‐atom of α‐aminophosphonates. The chiral diisopropyl (4R,5R)‐2‐chloro‐1,3,2‐dioxaphospholane‐4,5‐dicarboxylate ( 3 ) was found to be a good phosphonylating agent in this stereoselective reaction.     

Two New Iridoid Glycosides from Hedyotis tenelliflora Blume

Two new iridoid glycosides, teneoside A (=(2aR,5S)‐5‐[(β‐D ‐glucopyranosyl)oxy]‐2a,4a,5,7b‐tetrahydro‐4‐{[(α‐L ‐rhamnopyranosyl)oxy]methyl}‐1H‐2,6‐dioxacyclopenta[cd]inden‐1‐one; 1 ) and teneoside B (=methyl (1S,5R)‐1‐[(β‐D ‐glucopyranosyl)oxy]‐1,4a,5,7a‐tetrahydro‐5‐hydroxy‐7‐{[(α‐L ‐rhamnopyranosyl)oxy]methyl}cyclopenta[c]pyran‐4‐carboxylate; 2 ), were isolated from the roots of Hedyotis tenelliflora Blume , along with two known compounds, deacetylasperuloside ( 3 ) and scandoside methyl ester ( 4 ). Their structures were elucidated by chemical methods (acid hydrolysis) and spectroscopic analyses.     

Indium(III) Chloride‐Catalyzed Conversion of {[(Benzyloxy)carbonyl]amino}‐Substituted Sulfones with 2‐[(Trimethylsilyl)oxy]furan: A Facile Access to γ‐Butenolactone Derivatives Containing a Protected Amino Group

Treatment of {[(benzyloxy)carbonyl]amino}‐substituted sulfones 1 with 2‐[(trimethylsilyl)oxy]furan ( 2 ) in the presence of InCl₃ as a catalyst at room temperature produced the γ‐butenolactone derivatives 3 and 4 containing a protected amino group (Scheme 1). The products were formed in high yields (81–92%) within 3–10 h favoring the anti‐isomer 3 .     

Novel Fluoride‐Labile Nucleobase‐Protecting Groups for the Synthesis of 3′(2′)‐O‐Aminoacylated RNA Sequences

With the aim to develop a general approach to a total synthesis of aminoacylated t‐RNAs and analogues, we describe the synthesis of stabilized, aminoacylated RNA fragments, which, upon ligation, could lead to aminoacylated t‐RNA structures. Novel RNA phosphoramidites with fluoride‐labile 2′‐O‐[(triisopropylsilyl)oxy]methyl (=tom) sugar‐protecting and N‐{{2‐[(triisopropylsilyl)oxy]benzyl}oxy}carbonyl (=tboc) base‐protecting groups were prepared (Schemes 4 and 5), as well as a solid support containing an immobilized N⁶‐tboc‐protected adenosine with an orthogonal (photolabile) 2′‐O‐[(S)‐1‐(2‐nitrophenyl)ethoxy]methyl (=(S)‐npeom) group (Scheme 6). From these building blocks, a hexameric oligoribonucleotide was prepared by automated synthesis under standard conditions (Scheme 7). After the detachment from the solid support, the resulting fully protected sequence 34 was aminoacylated with L ‐phenylalanine derivatives carrying photolabile N‐protecting groups (→ 42 and 43 ; Scheme 9). Upon removal of the fluoride‐labile sugar‐ and nucleobase‐protecting groups, the still stabilized, partially with the photolabile group protected precursors 44 and 45 , respectively, of an aminoacylated RNA sequence were obtained (Scheme 9 and Fig. 3). Photolysis of 45 under mild conditions resulted in the efficient formation of the 3′(2′)‐O‐aminoacylated RNA sequence 46 (Fig. 4). Additionally, we carried out model investigations concerning the stability of ester bonds of aminoacylated ribonucleotide derivatives under acidic conditions (Table) and established conditions for the purification and handling of 3′(2′)‐O‐aminoacylated RNA sequences and their stabilized precursors.     

The synthesis of 8‐hydroxyquinazoline derivatives and their acid‐base interactions

The reaction of N‐(2‐R¹‐oxyphenyl)benzimidoyl chlorides with cyanamide derivatives in the presence of titanium tetrachloride as a catalyst has yielded some new 4‐amino‐8‐R¹‐oxy‐2‐phenylquinazolines. pK_a values have been determined for these compounds and the influence of substituents at the basicity of the parent system has been discussed. Some investigations on the methyl‐quinazolinyl ether cleavage in different medium have been done yielding the appropriate hydroxyquinazoline derivatives. In those cases when the deprotection of 4‐amino‐8‐methoxy‐2‐phenylquinazoline was carried in aqueous acidic solutions, the formation of the hydrolysis products 3,4‐dihydro‐2‐phenyl‐4‐quinazolone derivatives was observed as well.     

Two Antioxidant Alkaloids from Portulaca oleracea L.

Two alkaloids, oleraceins F and G, were isolated from Portulaca oleracea L., and their structures were determined as methyl (2S)‐6‐[(β‐D ‐glucopyranosyl)oxy]‐2,3‐dihydro‐5‐hydroxy‐1‐[(2E)‐3‐(4‐hydroxy‐3‐methoxyphenyl)prop‐2‐enoyl]‐1H‐indole‐2‐carboxylate and methyl (2S)‐6‐[(β‐D ‐glucopyranosyl)oxy]‐2,3‐dihydro‐5‐hydroxy‐1‐[(2E)‐3‐(4‐hydroxyphenyl)prop‐2‐enoyl]‐1H‐indole‐2‐carboxylate, based on their spectroscopic data. Oleraceins F and G exhibited scavenging activity against 1,1‐diphenyl‐2‐picrylhydrazyl (DPPH) radical, with EC₅₀ values of 21.00 and 37.69 μM , respectively.     

Three New Derivatives and Others Constituents from the Roots and Twigs of Trilepisium madagascariense DC

Three new compounds, trilepisflavene ( 1 ), trilepisdepsidone ( 2 ), and daturadiol stearate ( 3 ), together with nine known compounds, 2‐hydroxy‐4‐[(4‐hydroxy‐2‐methoxy‐6‐methylbenzoyl)oxy]‐6‐methylbenzoic acid ( 4 ), lichexanthone ( 5 ), naringenin ( 6 ), 3′,4′,5,7‐tetrahydroxyflavanone ( 7 ), 2‐hydroxybenzoic acid ( 8 ), methyl 2,4‐dihydroxy‐6‐methylbenzoate ( 9 ), β‐amyrin ( 10 ), eurothridiol palmitate ( 11 ), and β‐sitosterol ( 12 ), were isolated from the AcOEt extract of the twigs and the roots of Trilepisium madagascariense. Acetylation of eurothridiol palmitate was carried out and a new acetylated derivative ( 13 ) was obtained. The structures of the isolated and acetylated compounds were elucidated on the basis of spectroscopic analysis. Antimicrobial activity of all these compounds was evaluated using Mueller–Hinton broth (MHB) and Mueller–Hinton agar (MHA) method. Trilepisdepsidone , 2‐hydroxy‐4‐[(4‐hydroxy‐2‐methoxy‐6‐methylbenzoyl)oxy]‐6‐methylbenzoic acid, 3′,4′,5,7‐tetrahydroxyflavanone, and naringenin exhibited moderate to weak antimicrobial activity.