Spiro[pyrido[3,2,1‐ij]pyrimido[4,5‐b]quinoline‐7,5′‐pyrrolo[2,3‐d]pyrimidines] and Spiro[pyrimido[4,5‐b]quinoline‐5,1′‐pyrrolo[3,2,1‐ij]quinolines] Derived from 5,6‐Dihydro‐4H‐pyrrolo[3,2,1‐ij]quinoline‐1,2‐dione

Reaction of 5,6‐dihydro‐4H‐pyrrolo[3,2,1‐ij]quinoline‐1,2‐dione ( 1 ) with two equivalents of some 6‐aminouracils (or 6‐amino‐2‐thiouracil) generates spirocyclic tetrahydrobenzo[if]quinolizines ( 7 ). The one‐pot, three‐component reaction of amido ketone ( 1 ) with 6‐aminouracil (or 6‐amino‐2‐thiouracil) and a cyclic six‐membered 1,3‐diketone produces spirocyclic tetrahydropyrrolo[3,2,1‐ij]quinolinones ( 15 ).     

Three‐Component Reaction for Construction of Spiro[indoline‐3,7′‐thiazolo[3,2‐a]pyridines] and Spiro[benzo[4,5]thiazolo[3,2‐a]pyridine‐3,3′‐indolines]

The three‐component reaction of thiazole (benzothiazole), dialkyl but‐2‐ynedioate, and isatinylidene malononitriles in toluene at 110–120°C in a sealed tube afforded a mixture of cis/trans‐isomers of functionalized diastereoisomeric spiro[indoline‐3,7′‐thiazolo[3,2‐a]pyridines] and spiro[benzo[4,5]thiazolo[3,2‐a]pyridine‐3,3′‐indolines] in good yields. Both cis‐isomers and trans‐isomers were successfully separated out and fully characterized with spectroscopy and single crystal determination. Under similar conditions, the three‐component reaction containing 2‐(1,3‐dioxo‐1H‐inden‐2(3H)‐ylidene)malononitrile resulted in spiro[indene‐2,7′‐thiazolo[3,2‐a]pyridine] derivatives.     

Synthesis of substituted pyrimido[4,5‐b] and [5,4‐c]‐[1,8]naphthyridines

Ethyl 1‐ethyl‐7‐methyl‐4‐oxo‐1,4‐dihydro[1,8]naphthyridine‐3‐carboxylate ( 1 ), precursor of nalidixic acid, has been converted in two steps through ([1,8]naphthyridin‐3‐yl)carbonylguanidine derivatives into substituted pyrimido[4,5‐b] and [5,4‐c][1,8]naphthyridines.     

2,5‐Dimethyl‐6,7‐dihydrobenzo[h]pyrazolo[1,5‐a]quinazoline and 2‐tert‐butyl‐5‐methyl‐6,7‐dihydrobenzo[h]pyrazolo[1,5‐a]quinazoline

In both 2,5‐dimethyl‐6,7‐dihydrobenzo[h]pyrazolo[1,5‐a]quinazoline, C₁₆H₁₅N₃, (I), and 2‐tert‐butyl‐5‐methyl‐6,7‐dihydrobenzo[h]pyrazolo[1,5‐a]quinazoline, C₁₉H₂₁N₃, (II), which crystallizes with Z′ = 2 in the space group P, the non‐aromatic carbocyclic rings adopt screw‐boat conformations. The molecules of (I) are linked into chains of rings by a combination of C—H...N and C—H...π(arene) hydrogen bonds, while in (II) there are no hydrogen bonds of any kind.     

Synthesis of new benzo[h]‐ and benzo[f]chromeno[2,3‐b]‐pyridine‐5‐ones

A number of new benzo[h]‐ and benzo[f]chromeno[2,3‐b] pyridine‐5‐ones derivatives were synthesized from benzo[h]‐ and benzo[f]‐chromone‐carbonitriles and amino‐benzo[h]‐ and benzo[f]chromone‐carbaldehydes. © 2006 Wiley Periodicals, Inc. Heteroatom Chem 17:2–7, 2006; Published online in Wiley InterScience ( www.interscience.wiley.com ). DOI 10.1002/hc.20152     

Diphosphapodanden, [12]‐, [15]‐ und [18]Diphosphacoronanden,Diphosphacryptand‐8 und Alkalimetall‐Komplexe

Diphosphapodands, [12]‐, [15]‐, and [18]Diphosphacoronands, Diphosphacryptand‐8, and Alkali‐Metal Complexes The cyclizing bis‐phosphonium‐salt formation of the open‐chain bis‐phosphine 17a (1,1,7,7‐tetrabenzyl〈P.O.P‐podand‐7〉) with diethylene glycol derived dibromide 13a yields the 12‐membered cyclic bis‐phosphonium salt 20 (4,4,10,10‐tetrabenzyl‐12〈O.P.O.P‐coronand‐4〉‐4,10‐diium dibromide) in yields as high as 50–60%. The 1,1,10,10‐tetrabenzyl〈P.O₂.P‐podand‐10〉 17b forms with 13a the 15‐membered cyclic bis‐phosphonium salt 21 (7,7,13,13‐tetrabenzyl‐15〈O₂.P.O.P‐coronand‐5〉‐7,13‐diium dibromide) with the same high yield. By quaternization of the bis‐phosphine 17b with triethylene glycol derived dibromide 13b , the 18‐membered 7,7,16,16‐tetrabenzyl‐18〈O₂.P.O₂.P‐coronand‐6〉‐7,16‐diium dibromide 24 is obtained in 50% yield, too. The Wittig reaction of the cyclic phosphonium salts with benzaldehyde yields the 12‐, 15‐, and 18‐membered cyclic bis‐benzylphosphine dioxides 9, 10 , and 11 as cis‐ and trans‐isomers beside trans‐stilbene. The 7,13‐dioxido‐7,13‐dibenzyl‐15〈O₂.P.O₂.P‐coronand‐5〉 10 forms a crystalline 1 : 1 Na‐complex 23 , which exists as a dimer. The structure of 23 was established by an X‐ray analysis and spectroscopic data. The 7,16‐dibenzyl‐18〈O₂.P.O₂.P‐coronand‐6〉 28 that is available by reduction of 11 with CeCl₃/LiAlH₄ reacts with triethylene glycol derived dibromide 13b under Ruggly Ziegler‐dilution conditions to give the bicyclic bis‐phosphonium salt 29 (1,10‐dibenzyl〈P[O₂]₃.P‐cryptand‐8〉‐1,10‐diium dibromide) in 18% yield. Again, by the Wittig procedure with benzaldehyde, the 7,16‐dioxido〈P[O₂]₃P‐cryptand‐8〉 12 is obtained as the first diphosphacryptand. The FD‐MS (CH₂Cl₂) of the cyclic bis‐phosphine dioxides 10 – 12 show that they exist as [2M+Na]⁺ complexes. The complex formation constants K_a of 9 – 11 with alkali‐metal cations are studied and compared with the complex formation of corresponding crown ethers.     

Structural Transformation of Methoxy‐Substituted Benzo[de]benzo[4,5]imidazo[2,1‐a]isoquinolin‐7‐ones

Structural transformation of two methoxy derivatives of benzo[de]benzo[4,5]imidazo[2,1‐a]‐isoquinolin‐7‐one were determined via spectroscopic analysis. The transformation mechanism was proposed as the breakage and reformation of the lactam bond.     

Synthesis and reactions of 11H‐benzo[b]pyrano[3,2‐f]indolizines an pyrrolo[3,2,1‐ij]pyrano[3,2‐c]quinolines

2‐Methyl‐3H‐indoles 1 cyclize with two equivalents of ethyl malonate 2 to form 4‐hydroxy‐11H‐benzo[b]pyrano[3,2‐f]indolizin‐2,5‐diones 3, whereas 2‐mefhyl‐2,3‐dihydro‐1H‐indoles 9 give under similar conditions regioisomer 8‐hydroxy‐5‐methyl‐4,5‐dihydro‐pyrrolo[3,2,1‐ij]pyrano[3,2‐c]quinolin‐7,10‐diones 10 . The pyrone rings of 3 and 9 can be cleaved either by alkaline hydrolysis to give 7‐acetyl‐8‐hydroxy‐10H‐pyrido[1,2‐a]indol‐6‐ones 4 or 5‐acetyl‐6‐hydroxy‐2‐methyl‐1,2‐dihydro‐4H‐pyrrolo‐[3,2,1‐ij]quinolin‐4‐ones 11 , respectively. Chlorination of 3 and 9 with sulfurylchloride gives under subsequent ring opening 7‐dichloroacetyl‐8‐hydroxy‐10H‐pyrido[1,2‐a]indol‐6‐ones 5 or 5‐dichloracetyl‐6‐hydroxy‐2‐methyl‐1,2‐dihydro‐4H‐pyrrolo[3,2,1‐ij]quinolin‐4‐ones 12 . The dichloroacetyl group of 5 can be reduced with zinc to 7‐acetyl‐8‐hydroxy‐10H‐pyrido[1,2‐a]indol‐6‐ones 7. Treatment of the acetyl compounds 4, 7 and 11 with 90% sulfuric acid cleaves the acetyl group and yields 8‐hydroxy‐10H‐pyrido[1,2‐a]‐indol‐6‐ones 6 and 8 , and 6‐hydroxy‐2‐methyl‐1,2‐dihydro‐4H‐pyrrolo[3,2,1‐ij]quinolin‐4‐ones 13 . Reaction of dichloroacetyl compounds 12 with sodium azide yields 6‐hydroxy‐2‐methyl‐5‐(1H‐tetrazol‐5‐ylcarbonyl)‐1,2‐dihydro‐4H‐pyrrolo[3,2,1‐ij]quinolin‐4‐ones 14 via intermediate geminal diazides.     

Synthesis of novel benzo[h] [1,6]naphthyridines via a rearrangement of hexahydro‐5H‐pyrrolo [2,1 ‐c] [1,4]benzodiazepines

Heating of hexahydro‐5H‐pyrrolo[2,1‐c][1,4]benzodiazepine‐2,5,11‐trione in boiling phosphoryl chloride led to a rearranged product like 3,5‐dichlorobenzo[h][1,6]naphthyridine. This structure was established from X‐ray diffraction analysis.     

Synthesis of New tert‐Butyl‐ and Bromo‐functionalized [1,2,4]Triazino [5,6‐b]indole‐3‐thiols and Indolo[2,3‐b]quinoxalines

In the present investigation, the synthesis of a series of structurally new and interesting tert‐butyl‐ and bromo‐functionalized [1,2,4]triazino[5,6‐b ]indoles ( 6a – f ) and indolo[2,3‐b ]quinoxalines ( 8a – f ) has been achieved, involving the condensation reaction of 7‐bromo‐5‐tert‐butylisatins ( 4a – f ) with thiosemicarbazide ( 5 ) and benzene‐1,2‐diamine ( 7 ). The substrates 4a – f were prepared through bromination reaction of 5‐tert‐butylisatin ( 3 ) with NBS in PEG‐400 followed by alkylation reaction. The molecular structures of these newly synthesized compounds were elucidated on the basis of their elemental analyses and spectral data.     

One‐Pot Three‐Component Synthesis of 6H‐chromeno[4,3‐b] or Cyclopenta[b]furo[3,2‐f]quinoline Derivatives

Two series of furo[3,2‐f ]quinoline‐2‐carboxylate were obtained via a three‐component reaction of aldehydes, 5‐aminobenzofuran‐2‐carboxylate, and 4‐hydroxy‐2H‐chromen‐2‐one or cyclopentane‐1,3‐dione in DMF under catalyst‐free condition in high yields. This one‐pot three‐component reaction provided an efficient method for the synthesis of fused polycyclic heterocycles for bioactive screening.     

An Efficient Synthesis of Benzo[g]thiazolo[2,3‐b]quinazolin‐4‐ium and Benzo[g]benzo[4,5]thiazolo[2,3‐b]quinazolin‐14‐ium Hydroxides by a One‐pot,Three‐component Reaction under Green Conditions

A new series of benzo[g]thiazolo[2,3‐b]quinazolin‐4‐ium and benzo[g]benzo[4,5]thiazolo[2,3‐b]quinazolin‐14‐ium hydroxide derivatives have been synthesized by the one‐pot, three‐component reaction of aryl glyoxal monohydrates, 2‐hydroxy‐1,4‐naphthoquinone, and 2‐aminothiazole or 2‐aminobenzothiazole in the presence of triethylamine and p‐toluenesulfonic acid as organocatalysts in H₂O/acetone (2:1) at room temperature. This method offers mild reaction conditions, excellent yields, easy workup, and readily accessible starting materials and catalysts.     

Controlled Self‐Assembly by Mono‐p‐sulfonatocalix[n]arenes and Bis‐p‐sulfonatocalix[n]arenes

The complexation‐induced critical aggregation concentrations of 1‐pyrenemethylaminium by mono‐p‐sulfonatocalix[n]arenes and bis‐p‐sulfonatocalix[n]arenes (n=4, 5) were systemically measured by fluorescence spectroscopy. In all cases, the complexation‐induced critical aggregation concentration decreases by about 3 times upon addition of p‐sulfonatocalix[n]arenes. However, the optimal molar ratios for the aggregation of 1‐pyrenemethylaminium by mono‐p‐sulfonatocalix[n]arenes and bis‐p‐sulfonatocalix[n]arenes are distinctly different: For mono‐p‐sulfonatocalix[n]arenes, the optimum mixing ratio for the aggregation of 1‐pyrenemethylaminium is 1:4 mono‐p‐sulfonatocalix[n]arenes/1‐pyrenemethylaminium, whereas only 2.5 molecules of 1‐pyrenemethylaminium can be bound by one cavity of bis‐p‐sulfonatocalix[n]arenes. The intermolecular complexation of mono‐p‐sulfonatocalix[n]arenes and bis‐p‐sulfonatocalix[n]arenes with 1‐pyrenemethylaminium led to the formation of two distinctly different nanoarchitectures, which were shown to be nanoscale vesicle and rod aggregates, respectively, by using dynamic laser scattering, TEM, and SEM. This behavior is also different from the fiber‐like aggregates with lengths of several micrometers that were formed by 1‐pyrenemethylaminium itself above its critical aggregation concentration. Furthermore, the obtained nanoaggregates exhibit benign water solubility, self‐labeled fluorescence, and, more importantly, temperature responsiveness.     

On triazoles XLIX. Synthesis of 5,6‐dihydrothiazolo[3,2‐b]‐[1,2,4]triazol‐2‐yl‐, 6,7‐dihydro‐5H‐[1,2,4]triazolo[5,1‐b][1,3]thiazin‐2‐yl‐, and 5,6,7,8‐tetrahydro[1,2,4]triazolo[5,1‐b] [1,3]thiazepin‐2‐yl‐isoquinolinium salts

5′‐Mercapto‐1′H‐1,2,4‐triazol‐3′‐yl‐isoquinolinium salts (6) were synthesised by the reaction of ortho‐acyl phenylacetones (2) or the corresponding pyrylium salts (3) and 5‐amino‐2,3‐dihydro‐1H‐1,2,4‐triazole‐3‐thione (5) . Treatment of thioles 6 withα,ω‐dibromoalkanes led to type 15, 16 and 17 isoquinolinium salts condensed with thiazole, thiazine and thiazepine rings. When 6 are reacted with dibromomethane (10) 11 type dimeric structures are obtained.     

Straightforward Synthesis and Properties of Highly Fluorescent [5]‐ and [7]‐Helical Dispiroindeno[2,1‐c]fluorenes

This work presents a general approach for synthesis of substituted [5]‐helical dispiroindeno[2,1‐c]fluorenes based on Rh‐catalyzed intramolecular cyclotrimerization of triynes. This approach was further extended for the first synthesis of configurationally stable [7]‐helical dispiroindeno[2,1‐c]fluorenes. A series of variously substituted derivatives was prepared and their photophysical and electrochemical properties were evaluated. Their fluorescence emission maxima were in the region of 351–428 nm and quantum yields up to 88 % are the highest measured among the full‐carbon helical compounds.     

On the chemistry of 5‐aryl‐2‐hydrazino‐benzo[6,7]cyclohepta[1,2‐b]pyrido[2,3‐e] pyrimidin‐4‐one

Several pyrido[2,3‐e]pyrimidine fused with other rings have been prepared by intramolecular cyclization of 5‐(4‐chlorophenyl)‐2‐hydrazino‐benzo [6,7]cyclohepta‐[1,2‐b]pyrido[2,3‐e]pyrimidine‐4‐one ( 1 ) with acids, carbon disulfide to form triazole derivatives ( 2,4 ), halo‐ketones to give triazine derivative ( 5 ), β‐ketoesters, β‐cyanoesters, and β‐diketones to yield 2‐(1‐pyrazolyl) derivatives ( 7,9,10 ), and aldehydes to form arylhydrazone derivatives ( 11a,b ) which cyclized to form triazoles ( 12a,b ). Also, acyclic N‐nucleosides are prepared by heating under reflux 2‐hydrazino‐benzo[6,7]cyclohepta[1,2‐b]pyrido[2,3‐e] pyrimidin‐4‐one ( 1 ) with xylose and glucose to give the corresponding acyclic N‐nucleosides ( 13a,b ) which are cyclized to afford the corresponding protected tetra and penta–O‐acetate C‐nucleosides ( 14a,b ). Deacetylating of the latter nucleosides afforded the free acyclic C‐nucleosides ( 15a,b ). © 2007 Wiley Periodicals, Inc. Heteroatom Chem 18:34–43, 2007; Published online in Wiley InterScience ( www.interscience.wiley.com ). DOI 10.1002/hc.20248