Tricarbonyl iron complexes synthesis

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... 

Another recent example of sonochemical substitution is in the preparation of 7r-allyllactone(tricarbonyl)iron complexes, which are useful synthetic intermediates in the synthesis of lactones and lactams (185). Upon... 

Tricarbonyliron diene complexes have found many uses in synthetic chemistry but their synthesis is often not easy. Knolker has developed a range of tricarbonyl(7] -l-aza-l,3-butadiene) iron complexes that are excellent transfer agents for the Fe(CO)3 complexation of 1,3-dienes, and showed their versatility. As an extension to this work, Knolker and Gonser have prepared a polymer-supported l-aza-l,3-butadiene 321 by reaction of Merrifield s resin with phenolic l-aza-l,3-butadiene 320, formed from cinnamaldehyde and /> ra-hydroxyaniline (Scheme 105). The corresponding tricarbonyl iron complex 322 was formed by treatment of 321 with an excess of Fe2(CO)9 in THF using ultrasound. The iron complex was subsequently used efficiently as a transfer agent for the tricarbonyliron complexation of 1,3-dienes. 

Scheme 1.44 Tricarbonyl iron-complexed dendralenes enabling the synthesis of a formal terminal single DA-adduct of [4]dendralene [89],...

The synthesis of 1 -benzothiepin 1 -oxide (23) can be achieved via complex formation with tricarbonyl iron, and quantitative oxidation of the coordination compound 22 with 3-chloroperoxy-benzoic acid. Subsequent irradiation at — 50 C provides 23, which crystallized as yellow needles after low-temperature (-40 C) chromatography, and was characterized by 1H NMR spectroscopy at — 30 C23 before loosing sulfur within one hour at 13°C to give naphthalene. 

Tricarbonyliron-coordinated cyclohexadienylium ions 569 were shown to be useful electrophiles for the electrophilic aromatic substitution of functionally diverse electron-rich arylamines 570. This reaction combined with the oxidative cyclization of the arylamine-substituted tricarbonyl(ri -cyclohexadiene)iron complexes 571, leads to a convergent total synthesis of a broad range of carbazole alkaloids. The overall transformation involves consecutive iron-mediated C-C and C-N bond formation followed by aromatization (8,10) (Schemes 5.24 and 5.25). 

Over the past 15 years, we developed three procedures for the iron-mediated carbazole synthesis, which differ in the mode of oxidative cyclization arylamine cyclization, quinone imine cyclization, and oxidative cyclization by air (8,10,557,558). The one-pot transformation of the arylamine-substituted tricarbonyl(ri -cyclohexadiene) iron complexes 571 to the 9H-carbazoles 573 proceeds via a sequence of cyclization, aromatization, and demetalation. This iron-mediated arylamine cyclization has been widely applied to the total synthesis of a broad range of 1-oxygenated, 3-oxygenated, and 3,4-dioxygenated carbazole alkaloids (Scheme 5.24). 

In the quinone imine cyclization of iron complexes to carbazoles, the arylamine-substituted tricarbonyl(ri -cyclohexadiene)iron complexes 571 are chemoselectively oxidized to a quinone imine 574 prior to cyclodehydrogenation. This mode of cyclization is particularly applicable for the total synthesis of 3-oxygenated tricyclic carbazole alkaloids (Scheme 5.25). 

Using a one-pot process of oxidative cyclization in air, the arylamine 780a was transformed to the tricarbonyl(ri -4b,8a-dihydro-9H-carbazole)iron complex 792. Finally, demetalation of 792 and subsequent aromatization gave carbazomycin A (260). This synthesis provided carbazomycin A (260) in three steps and 65% overall yield based on 602 (previous route four steps and 35% yield based on 602) (610) (Scheme 5.88). 

The arylamine 794 required for the improved total synthesis of carbazomycin B (261) was prepared in quantitative yield by hydrogenation of the nitroaryl derivative 793 (see Scheme 5.85). Oxidative coupling of the iron complex salt 602 and the arylamine 794 in air afforded the tricarbonyl(ri -4b,8a-dihydro-9H-carbazole)iron complex (795). Demetalation of 795, followed by aromatization, led to O-acetylcarbazomycin B (796). 

Iron carbonyls have been used in stoichiometric and catalytic amounts for a variety of transformations in organic synthesis. For example, the isomerization of 1,4-dienes to 1,3-dienes by formation of tricarbonyl(ri4-l,3-diene)iron complexes and subsequent oxidative demetallation has been applied to the synthesis of 12-prostaglandin PGC2 [10], The photochemically induced double bond isomerization of allyl alcohols to aldehydes [11] and allylamines to enamines [12,13] can be carried out with catalytic amounts of iron carbonyls (see Section 1.4.3). 

Chemoselective oxidation of 4-methoxyanilines to quinonimines can be achieved in the presence of tricarbonyl(ri4-cyclohexadiene)iron complexes. This transformation has been used for the synthesis of carbazoles via intermediate tricarbonyliron-coordinated 4b,8a-dihydrocarbazol-3-one complexes (Scheme 1.24) [57]. 

The first aspect is illustrated by the synthesis of tricarbonyl(ri4-l,3-diene)iron complexes from pentacarbonyliron in the presence of catalytic amounts of a 1-azabuta-... 

Cyclobutadiene iron tricarbonyl complexes can be isolated and have been utilized in organic synthesis. Both intra- and intermolecular [2 + 2] cycloadditions of alkenes with cyclobutadiene complexes are observed upon decomplexation using CAN or TMANO (Schemes 164-165). The stereochemistry of the aUcene is retained in the product. Iron tricarbonyl diene complexes are compatible with metathesis reactions... 

While a great number of tricarbonyl( -diene)iron complexes have been reported and their reactivity investigated, much less is known of the corresponding heterodiene complexes. In recent years, synthesis of several tricar-bonyl(heterodiene)iron systems involving r] coordination of the heterodiene unit has been achieved. Among the tetracarbonyl(/ -olefin)iron complexes prepared by Weiss was tetracarbonyl(cinnamaldehyde)iron, which converts on heating to the //-bonded tricarbonyl(cinnamaldehyde)iron. The preparation and synthetic utility of (benzylideneacetone)tricarbonyl iron, an analogous complex of an ar,/9-unsaturated ketone, are reported here. 

The complex functions as a convenient source of the tricarbonyliron moiety by displacement of the unsaturated ketone. For example, reaction with 1,3-cycloheptadiene results in a 78% yield of (//-l,3-cycloheptadiene)tricar-bonyliron. More importantly, it may be used in syntheses of tricarbonyl-(diene)iron complexes where the iron carbonyls are not satisfactory. Several complexes of sensitive heptafulvenes have been prepared in this way, and the reagent has been used in the synthesis of tricarbonyliron complexes of several steroids. 

A useful synthesis of racemic methyl lipoate from the key intermediate 348, prepared via a six-step reaction sequence, starts from tricarbonyl(diene)iron complex 350 (Scheme 67) <1998EJ01949>. The main goal of this practical method, based on the use of the optically active iron complex 350, was a possible stereoselective synthesis of LA and other structural analogues. 

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