Heterocyclic Ring -Complexes

Heterocyclic ring complexes, and boron-containing rings, 3,42 Hetero-[4+3]-cycloadditions, characteristics, 10, 617 j5-Heterocyclopentadienyl complexes, with platinum, rf-boron-carbon ligands, 8, 663... 

Inclusion of bismuth atoms in heterocyclic ring complexes has been actively investigated for a number of years. Complexes of the type (17), for example, l-phenyl-2,5-dimethylbismole, have been sought for comparison with pyrrole derivatives and for information about the degree of aromaticity in its heavier analogs. Compound (17) is prepared via the addition of 2(Z),5(Z)-dilithio-3,4-dimethylhexa-2,4-diene to PhBil2 in 28% yield. This heterocycle is converted to the dibismuthine in the standard fashion treatment of (17) with Na in liquid NH3 followed by addition of 1,2-dichloroethane. 

Diels-Alder reactions, 4, 842 flash vapour phase pyrolysis, 4, 846 reactions with 6-dimethylaminofuKenov, 4, 844 reactions with JV,n-diphenylnitrone, 4, 841 reactions with mesitonitrile oxide, 4, 841 structure, 4, 715, 725 synthesis, 4, 725, 767-769, 930 theoretical methods, 4, 3 tricarbonyl iron complexes, 4, 847 dipole moments, 4, 716 n-directing effect, 4, 44 2,5-disubstituted synthesis, 4, 116-117 from l,3-dithiolylium-4-olates, 6, 826 electrocyclization, 4, 748-750 electron bombardment, 4, 739 electronic deformation, 4, 722-723 electronic structure, 4, 715 electrophilic substitution, 4, 43, 44, 717-719, 751 directing effects, 4, 752-753 fluorescence spectra, 4, 735-736 fluorinated derivatives, 4, 679 H NMR, 4, 731 Friedel-Crafts acylation, 4, 777 with fused six-membered heterocyclic rings, 4, 973-1036 fused small rings structure, 4, 720-721 gas phase UV spectrum, 4, 734 H NMR, 4, 7, 728-731, 939 solvent effects, 4, 730 substituent constants, 4, 731 halo... 

The successful application of heterocyclic compounds in these and many other ways, and their appeal as materials in applied chemistry and in more fundamental and theoretical studies, stems from their very complexity this ensures a virtually limitless series of structurally novel compounds with a wide range of physical, chemical and biological properties, spanning a broad spectrum of reactivity and stability. Another consequence of their varied chemical reactivity, including the possible destruction of the heterocyclic ring, is their increasing use in the synthesis of specifically functionalized non-heterocyclic structures. 

The chemistry of furazans and furoxans has been the subject of intensive investigations over the years. There has been been a substantial increase in synthetic manipulations of substituents attached to these ring systems. Additionally, there are a number of publications that deal with the incorporation of the heterocyclic rings into more complex molecules. It is the aim of this review to present new synthetic developments and to update reviews in the field of... 

Esters of diphenylacetic acids with derivatives of ethanol-amine show mainly the antispasmodic component of the atropine complex of biologic activities. As such they find use in treatment of the resolution of various spastic conditions such as, for example, gastrointestinal spasms. The prototype in this series, adiphenine (47), is obtained by treatment of diphenyl acetyl chloride with diethylaminoethanol. A somewhat more complex basic side chain is accessible by an interesting rearrangement. Reductive amination of furfural (42) results in reduction of the heterocyclic ring as well and formation of the aminomethyltetrahydro-furan (43). Treatment of this ether with hydrogen bromide in acetic acid leads to the hydroxypiperidine (45), possibly by the intermediacy of a carbonium ion such as 44. Acylation of the alcohol with diphenylacetyl chloride gives piperidolate (46). ... 

Antidepressant activity is retained when the two carbon bridge in imipramine is replaced by a larger, more complex, function. Nucleophilic aromatic substitution on chloropyridine 31 by means of p-aminobenzophenone (32) gives the bicyclic intermediate 33. Reduction of the nitro group (34), followed by intramolecular Schiff base formation gives the required heterocyclic ring system 35. Alkylation of the anion from 35 with l-dimethylamino-3-chloropropane leads to tampramine 36 [8]. 

---