Gold-catalyzed cyclization of enediynes and arenediynes to 6H-benzo[c]chromen-6-one and dibenzo[c,h]chromen-6-one derivatives

The efficient synthesis of 6H-benzo[c]chromen-6-one and dibenzo[c,h]chromen-6-one derivatives is described. Thus, treatment of arenediynes 1 and enediynes 5 with 5?mol % Ph₃PAuCl and 10?mol % of AgSbF₆ in refluxing toluene gave dibenzo[c,h]chromen-6-ones 4 and 6H-benzo[c]chromen-6-ones 6, in good yields, respectively.     

Synergistic effects of macrocyclic polyethers and converging anionic binding sites : Synthesis of biphenyl crown ethers and lipophilization of divalent cations

The synthesis of nine novel macrocyclic polyethers with a 1,1'-biphenyl subunit is described. Crown ethers 2,4,5 and 7 have substituents with terminal acid groups at the 4- and 4'- positions of the 1,1'-biphenyl subunit and crown ethers 9, 11, 12 and 14 have similar substituents at the 3- and 3'-positions. In the ionic form these crown ethers extract divalent cations (Ca²⁺, Sr²⁺ and Ba²⁺) from basic aqueous solutions into chloroform. The degree of lipophilization varies with the size of the cation and of the crown ether cavity, with the position and the length of the substituents and with the nature of the terminal acid groups. ¹H NMR spectroscopic data of the complexes in chloroform are in agreement with a structure of the complexes in which the cation is encapsulated by oxygen atoms and anionic groups.     

Vicinal phenyl group shift in the lead tetraacetate and related oxidations of 5,5,5-triphenyl-1-pentanol

In the lead tetraacetate and heavy metal-bromine oxidations of 5,5,5-triphenyl-1-pentanol 1d, the major cyclization product obtained was the rearranged 2,2,3-triphenyltetrahydro-2H-pyran 11d, resulting from homolytic and heterolytic 1,2-phenyl group shift (the latter only in the lead tetraacetate reaction) in the respective intermediate species with electron deficient δ-carbon 4d and 6d.     

Generation of dienone and trienone dianion derivatives : Double deprotonation as a route to lumo-filled π-systems

Conjugated unsaturated carbonyl compounds and their analogues 1 are a^1,3,5...-reagents. An umpolung of this intrinsic reactivity can be achieved by generation of the dianions 2, LUMO filled π-systems, from hydrogenated precursors, see schemes 1 and 2. The preparation of the allylated ketones 3a–d, of the acid derivatives 3e–h, 9, 10, 12 as well as of the dienones 11 is described. Their double deprotonation (→14, 18, 26, 30, 33, 36, and 40) is carried out by sequential treatment with potassium hydride and s-butyllithium/tetramethylethylene diamine (TMEDA) in THF. The decisive role of potassium in the second deprotonation step is demonstrated (Table 1 and eqn (6)). The brightly colored suspensions or solutions of these Li/K-dianions were quenched with the electrophile benzophenone. The products (15, 20, 27, 31, 34, 37, 41) result exclusively from ω-reactivity (d⁵- and d⁷reactivity) of the ambident dianionic nucleophiles (cf formulae 2, n = 2,3).     

Reactions of β-substituted amines-IV: Kinetics and stereochemistry of the thermal to (r) 3-chloro-1-ethylpiperidine,and the stereo-chemical course of their reactions with nucleophiles

The rate of the thermal rearrangement of (S) 2 chloromethyl-1-ethylpyrrolidine [(S)-1a] to (R)-3-chloro-1-ethylpiperidine [(R) 2a] has been examined at three temperatures in benzene by PMR and polarimetry. The rearrangement was shown to be completely stereospecific and to obey a simple first order rate law. The calculated E_a ΔH3 and ΔS3 were 22 ± 2 $\text{kcal}\text{mole}$ (25°), 21 ± 2.5 $\text{kcal}\text{mole}$ (25°) and - 10 ± 2 e.u. (0°K) respectively. The effect of solvents having differing dielectric constants was also studied. A transition state 9'a and an ion pair intermediate 3a are suggested for the rearrangement. The stereochemical course of the reactions of (S)-1a, (R)-2a and (S)-2a with hydroxide and methoxide ions have been shown to be 100% stereospecific with an uncertainty of about 1%. The absolute configurations of all optically active reactants and products [(S)- and (R)-4a, (S)-4b (R)- and (S)-5a, (R)-5b, (S,S')-6a, (S,R')-7a and (R,R')-8a] were established by chemical correlations with known compounds or by ORD and chemical inference. The ring opening of both the primary and secondary aziridinium ion positions of 1-azonia-1-ethylbicyclo [3.1.0]hexane [(S)-3a] by nucleophiles proceeds entirely by S_N2 processes. The conversion of (R)-1-ethyl-3-hydroxypiperidine [(R)-5a] to (S)-2a. HCl with thionyl chloride in chloroform proceeds by inversion with 4.8% racemization, whereas the thermal rearrangement of (S)-1a to (R)-2a occurs with complete retention of absolute configuration.     

Cyclophanes—VII : Conformations of [2.2](2,5)furanoparacyclophane,[2.2](2,5)furano(1,4)naphthalenophane and [2.2](2,5)furano(9,10)anthracenophane. perpendicularity of aromatic moieties

Variable temperature NMR spectroscopy was used to study the conformational behavior of [2.2](2,5)furanoparacyclophane (1), [2.2](2,5)furano(1,4)naphthalenophane (2) and [2.2](2,5)furano(9,10)anthracenophane (3). While the method was useful in studying 1, it was not adequate for 2 and 3. Variable temperature UV absorption and fluorescence emission studies provided information on the conformations of 2 and 3. The UV absorption and emission spectra of 1 were blue-shifted relative to their ambient temperature spectra. Those of 2 were not shifted at all and those for 3 were red-shifted. The data is consistent with an anti-orientation of the aromatic rings in 2 both at ambient and low temperture. The aromatic rings in 3 are perpendicular to one another at low temperature and probably at room temperature as well. Exiplex bands were absent in the room temperature emission spectra of 1, 2 and 3 as well as the low temperature spectra of 2 and 3. An exciplex band was observed in the low temperature emission spectrum of 1.     

Macroexpansion methodology : Medium ring synthesis based on an eight unit ring expansion process

Treatment of 1,2-(E,E)-di(1-buta-1,3-dienyl)cyclohexanol (21) with potassium hydride in tetrahydrofuran at room temperature resulted in the facile formation of a 14-membered ring dienolate which on kinetic protonation provided cyclotetradeca-3,5,7-trien-1-one. This novel rearrangement which provides the basis for an efficient, eight unit ring expansion method was also observed when 5,8-dimethyl-5-hydroxy-1,3,7,9-decapentaene (28), the acyclic analogue of 21, was treated with potassium hydride in tetrahydrofuran. Methodology for the preparation of 21 and 28 including the preparation of 1-lithio-1,3-butadiene is also described.     

Structure-reactivity relationship in the solvolysis of 5,10-secosteroidal 5-p-nitrobenzoates1

The solvolysis of (Z)- and (E)-3β-acyloxy-5,10-seco-1(10)-cholesten-5β-ol p-nitrobenzoates 4 and 5 has been investigated and compared with the solvolytic reactivity of the epimeric (Z)- and (E)-5α-p-nitrobenzoates 1 and 2, as well as of the reference compound, i.e. the 1,10-saturated 5α-p-nitrobenzoate. Kinetic data and product analysis revealed that the relative spatial orientation of the 1(10)-olefinic double bond and the chiral center at C(5) in the 10-membered ring, which these secosteroidal 5-p-nitrobenzoates can adopt in the transition state, is the main factor which determines their solvolytic behaviour, so that the esters 1,2 and 5 solvolyse with transannular double bond participation, while such an interaction is not present in the case of the (Z)-5β-ester 4.     

Circular dichroism of some cyclopropane ring containing 1,3-cyclo-5,10-seco-steroidal ketones

Circular dichroism of the rearranged keto steroids 3 and 4, containing a condensed three and nine-membered ring system, shows that the conformation of the nine-membered ring is the same in solution as in the crystal; reduction of the kto group does not change this situation. CD also indicates that epimerization at C(5) in the pair $\text{7}\text{8}$ and the pair $\text{11}\text{12}$ leaves the cyclononanone ring conformation unchanged.     

N-(6,7-methylenedioxy-3-quinazolinio)amidates—I synthesis spectra and some dark reactions

The title compounds 5 and/or their dimers 6, obtained by ring closure of the diacyl derivatives 4, exist in monomeric and dimeric forms in aprotic solvents, the positions of equilibria being dependent on the nature of the substituents and solvent. In several cases the pure monomeric and dimeric forms were obtained in the crystalline state. In protic solvents adducts of types 7 and 12 are formed, some of which are stable in the crystalline state. IR, NMR and mass spectra of compounds 5–7 and 12, and several dark reactions, are discussed.     

Total synthesis,reactivity, and structural clarification of lindenatriene

The synthesis of lindenatriene (1) and iso-lindenatriene (12) were achieved, along with the des-hydroxy model compounds (10 and 18, respectively), and compared to reported ¹H NMR spectra in the literature (1a and 10a). These comparisons clarify the correct initial assignment of lindenatriene (1) as well as its instability and propensity to isomerize into the more thermodynamically favored iso-lindenatriene (12).     

A template guided approach to generating cell permeable inhibitors of Staphylococcus aureus biotin protein ligase

Inhibitors of biotin protein ligase (BPL) are novel antimicrobial compounds with the potential to treat infections caused by bacteria resistant to current antibiotics. A novel BPL inhibitor (12, K_i 1.4 μM) was synthesized from biotin acetylene and an azide-functionalized analogue of fluorescent nitrobenzofurazan by Cu(I) catalysed cycloaddition and also by template guided synthesis using wild-type BPL from Staphylococcus aureus. LC/HRMS-based detection provides improved sensitivity over previous reports using a mutant BPL, with demonstrated applicability to other BPLs. Super-imaging fluorescence microscopy demonstrated the accumulation of 12 in the cytoplasm of S. aureus, but not Escherichia coli. This novel fluorescent probe can be used to gain new insights into the mechanism of uptake, efflux and metabolism of BPL inhibitors in S. aureus.     

The NMR spectra of porphyrins—14: Self-aggregation of zinc(II) meso-nitro and meso-dinitro octaethylporphyrins

Complex formation in zinc(II) meso-nitro-octa-ethylporphyrin (1) and the corresponding α,β-dinitro (2) and α, γ-dinitro (3) zinc(II) chelates has been studied using proton NMR at 220MHz. This allows complete resolution of all the distinct groups in the proton spectrum, and the large concentration dependence of the spectra of 1 and 2 can be analysed to afford the monomeric and monomer-dimer shifts for all protons in these molecules. In contrast 3 shows no concentration dependence, nor any change upon addition of pyrrolidine, which immediately dissociates the aggregates of 1 and 2. The monomeric ¹H and ¹³C shifts are reported, together with those of zinc(II) octaethylporphyrin (4), and the complete assignment given allows the substituent shifts of the meso nitro groups in the porphyrin to be obtained. Analysis of the monomer-dimer shifts in terms of the ring current model gives the detailed geometries of the dimers, which have an inter-ring separation of ca 4.5 Å and a lateral displacement from the vertical of ca 1.0 Å. The results also allow the distinction between two different molecular complexes considered previously, and fully confirm our earlier suggestions that binding is due to metal-to-porphyrin, rather than metal-to-substituent, interactions.     

Efficient synthesis of 3-benzoyl Benzo[b]thiophenes and raloxifene via Mercury(II)-Catalyzed cyclization of 2-alkynylphenyl alkyl sulfoxides

The unique selective estrogen receptor modulator, Raloxifene (1), and antitubulin agent 2 were synthesized through the key intermediate, 4-methoxybenzyl 2-bromo-4-methoxyphenyl sulfoxide (6), respectively. It was found that compared with the o-sulfanyl aryl bromides, the sulfinyl group at ortho position accelerated the Sonogashira coupling reaction of aryl bromides. Thus, compound 6 was coupled with 3,4,5-trimethoxyphenyl acetylene, followed by mercury-catalyzed cyclization reaction afford compound 2 in 79% overall yield. Raloxifene (1) was prepared from compound 6 in four steps and 33% overall yield via coupling reaction with 1-trimethylsily-2-(4-tert-butyldimethylsiloxy)phenylethyne, mercury-catalyzed cyclization reaction, alkylation and demethylation.     

Bile pigment studies—III: Controlled oxidative degradation of 1,19(21,24h)-bilindiones (bilitrienes)

Treatment of the model 1,19(21,24$\text{H}$)-bilindione (1) with thallium(III) acetate in methanol gives the thallium(III) complex (11) which is unstable and in the presence of air and methanol is transformed into the 15,16-dimethoxy complex (12), characterised as the metal free derivative (13). When exposed to light, solutions of (12) are oxidised to afford, after work-up, the 14-formyl-1(15$\text{H}$)-tripyrrinone (4) and ethylmethylmaleimide (17). A general discussion of mechanistic implications is presented.     

Aromatization-driven Grob-fragmentation approach toward polyazaacenes. Synthesis and amination of multi-functionalized diazapentacenes

A general approach toward the synthesis of multi-functionalized diazapentacene derivatives 1, using 1,2,3,4-tetrachloro-5,5-dimethoxycyclopentadiene (TDCp, 2), a substituted benzene-1,2-diamine (ADA, 6), and a naphthalene-1,4-dione (BQ, 3) as the building units, is described. The synthesis basically entails three operations: (i) oxidation of the dichloroetheno-bridge in the Diels-Alder cycloadduct 4 of TDCp and 3, (ii) condensation of the 1,2-diketone 5 thus generated with an ADA to give quinoxaline-fused polycyclic compounds 7, followed by (iii) an one-pot, three-reaction process keyed upon the base- or acid-catalyzed aromatization-driven Grob-type fragmentation to produce quinoxaline ring-embedded diazapentaceneesters 1. The diazapentacene derivative 1a underwent the nucleophilic aromatic ipso-amination with primary and secondary amines to afford the amino-substituted derivatives 12, which tend to self-assemble in solid state driven by the cofacial π-stacking interactions, demonstrated by the crystal packing structures of 12a and 12f.     

Synthesis of 2,3,4-trideoxy-4-c-(phenylphosphinyl)-dl-glycero-pentofuranose and its 1,5-diacetate

Synthesis of 2,3,4-trideoxy-4-C-(phenylphosphinyl)-dl-glycero-pentofuranose (11) starting from 2-furanmethanol was successful. The reaction of methyl 2,3-dideoxy-(1S)-dl-pentopyranosid-4-ulose 4-(p-toluenesulfonylhydrazone) with methyl phenylphosphonite gave methyl (4RS)-2,3,4-trideoxy-4-C-[(methoxy)phenylphosphinyl]-4-C-(p-toluenesulfonylhydrazino)-(1S)-dl-pentopyranoside (7), which on treatment with sodium borohydride afforded methyl 2,3,4-trideoxy-4-C-[(methoxy)phenylphosphinyl]-(1S)-dl-glycero-pentopyranoside (9). Treatment of compound 9 with SDMA followed by hydrolysis and treatment with acetic anhydride-pyridine afforded 1,5-diacetate 12 of compound 11.     

Reaction of η5-cyclopentadienylbis(triphenylphosphine)cobalt(I) with alkadiynes. Preparation and reactions of bicyclic cobalt metallocycles and a stable trimethylsilyl-substituted mono-complexed alkadiyne. Comments on the mechanism of cobalt-catalyzed alkyne cooligomerization

Reactions of η⁵-cyclopentadienylbis(triphenylphosphine)cobalt(I) (5) with several 2,n-alkadiynes (2) were investigated. Each of these reactions leads initially to a material in which one of the acetylene functional groups is π-coordinated to cobalt; this complex then undergoes conversion to a metallocycle. In cases where the two acetylene functions are connected by three- and four-carbon bridges (2b, 2c), metallocycles formed by intramolecular reaction of two acetylene functions in the same molecule may be isolated. In cases where the acetylene functions are joined by larger or smaller bridges, the reactions are more complex, and both inter- and intramolecular metallocycles are formed. Reactions of 5 with 1,8-bis(trimethylsilyl)-1,7-octadiyne (16) gives an isolable crystalline mono-acetylene complex (17), this material is stable in the solid state but undergoes conversion to metallocycle (18) in benzene solution. The relationship of these results to the mechanism of the CpCo(CO)₂-catalyzed benzocycloalkene synthesis is discussed; it is suggested that intramolecular metallocycles are intermediates in reactions leading to benzocyclopentanes and -cyclohexenes, but intermolecular metallocycles are probably involved in reactions leading to benzocyclobutenes.     

A convenient synthesis of 1α- and 1β-hydroxycholesterol

An efficient procedure for the preparation of 1α-hydroxycholesterol 3-acetate 4 is described, which starts from cholesterol and involves as key steps transannular cyclization of the ten-membered ring ontaining (E)-3β-acetoxy-5,10-seco-1(10)-cholesten-5-one 1 to the oxetane derivative 1α,5-epoxy-5α-cholestan-3β-ol acetate 3, and opening of the four-membered ether ring in the latter compound. 1β-Hydroxycholesterol diacetate 9 was obtained by oxidation of 4 to the 1-oxo derivative 8, followed by metal hydride reduction and acetylation.     

31P Solid state NMR geometrical effects on the chemical shift tensor

The principal components of the ³¹P chemical shift tensor σ of four cyclic organophosphorus compounds of different size, where the phosphorus atoms have the same chemical environment are reported from solid state NMR studies. The σ tensors show a large anisotropy. The asymmetry parameter η shows a linear variation as a function of the intracyclic bond angle around the phosphorus.