Aromatization rearrangement, skeletal

Benzene formation from all isohexanes had a similar energy of activation value. With platinum this was nearly twice as high as that of n-hexane aromatization (62) with palladium black, however, nearly the same values were found for -hexane and isohexanes (97a). This indicates a common rate-determining step for aromatization with skeletal rearrangement. This is not the formation and/or transformation of the C5 ring. We attribute benzene formation to bond shift type isomerization preceding aromatization. It requires one step for methylpentanes and two steps for dimethyl-butanes this is why the latter react with a lower rate, but with the same energy of activation. 

A book (B-71MS) and a review by Nishiwaki (74H(2)473) contain much information about the behaviour of pyrazoles under electron impact. The Nishiwaki review covers mainly the hydrogen scramblings and the skeletal rearrangements which occur. One of the first conclusions reached was that pyrazoles, due to their aromatic character, are extremely stable under electron impact (67ZOR1540). In the dissociative ionization of pyrazole itself, the molecular ion contributes about 45% to the total ion current thus, the molecular ion is the most intense ion in the spectrum. 

Reforming is the conversion primarily of naphthenes and alkanes to aromatics, but other reactions also occur under commercial conditions. Platinum or platinum/rhenium are the hydrogenation/ dehydrogenation component of the catalyst and alumina is the acid component responsible for skeletal rearrangements. 

Because of Us high polarity and low nucleophilicity, a trifluoroacetic acid medium is usually used for the investigation of such carbocationic processes as solvolysis, protonation of alkenes, skeletal rearrangements, and hydride shifts [22-24] It also has been used for several synthetically useful reachons, such as electrophilic aromatic substitution [25], reductions [26, 27], and oxidations [28] Trifluoroacetic acid is a good medium for the nitration of aromatic compounds Nitration of benzene or toluene with sodium nitrate in trifluoroacetic acid is almost quantitative after 4 h at room temperature [25] Under these conditions, toluene gives the usual mixture of mononitrotoluenes in an o m p ratio of 61 6 2 6 35 8 A trifluoroacetic acid medium can be used for the reduction of acids, ketones, and alcohols with sodium borohydnde [26] or triethylsilane [27] Diary Iketones are smoothly reduced by sodium borohydnde in trifluoroacetic acid to diarylmethanes (equation 13)... 

Open chain hydrocarbons, skeletal rearrangements, 29 298-302 aromatic selectivities, 29 302 atomization, 29 298-302 cyclization, 29 298-302 Open sequence in reaction mechanisms, 32 ... 

A common feature of any cyclization reaction is that a new intramolecular C—C bond is produced that would not have been formed in the absence of the catalyst. Those reactions in which one ring closure step is sufficient to explain the formation of a given cyclic product will be called simple cyclization processes, although their mechanism is, as a rule, complex. We shall distinguish those cases in which any additional skeletal rearrangement step(s) is (are) required to explain the process. Some specific varieties of hydrocarbon ring closure processes are not included. A recent excellent review deals with the formation of a second ring in an alkyl-substituted aromatic compound (12). Dehydrocyclodimerization reactions have also to be omitted—all the more since it is doubtful whether a metallic function itself is able to catalyze this process (13). 

Aromatization of dihalocarbene adducts to 1,4-cyclohexadiene or synthetic equivalents is the method of choice for the synthesis of the parent benzocyclo-propene (1). ° The mechanism of the aromatization step of the intermediate 7,7-dihalogenobicyclo[4.1.0]hept-2-ene (51) has been shown by labeling experiments with 51 depleted of C at Cl, to proceed via a series of elimination and double bond migration steps via cyclopropene- and alkylidenecyclopropane intermediates 52 to 54 with preservation of the original carbon skeleton. The synthesis of the benzannelated homologue, l//-cyclopropa[b]naphthalene (42), by the same route confirms these findings. Some skeletal rearrangement has, however, been observed in an isolated case. ... 

A long-established feature of the carbocation intermediates of reactions, such as SnI solvolysis and electrophilic aromatic alkylation, is a skeletal rearrangement involving a 1,2-shift of a hydrogen atom, or an alkyl, or aryl group. The stable ion studies revealed just how facile these rearrangements were. Systems where a more stable cation could form by a simple 1,2-shift did indeed produce only that more stable ion even at very low temperatures (see, e.g., Eq. 3). 

Very little skeletal rearrangement occurs via pyrolysis, a fact inherent in the failure of free radicals to readily isomerize by hydrogen atom or alkyl group migration. As a result, little branched alkanes are produced. Aromatization through the dehydrogenation of cyclohexanes and condensation to form polynuclear aromatics can take place. Additionally, olefin polymerization also can occur as a secondary process. 

Catalytic reforming92-94 of naphthas occurs by way of carbocationic processes that permit skeletal rearrangement of alkanes and cycloalkanes, a conversion not possible in thermal reforming, which takes place via free radicals. Furthermore, dehydrocyclization of alkanes to aromatic hydrocarbons, the most important transformation in catalytic reforming, also involves carbocations and does not occur thermally. In addition to octane enhancement, catalytic reforming is an important source of aromatics (see BTX processing in Section 2.5.2) and hydrogen. It can also yield isobutane to be used in alkylation. 

The acid-catalyzed isomerization of cycloalkenes usually involves skeletal rearrangement if strong acids are used. The conditions and the catalysts are very similar to those for the isomerization of acyclic alkenes. Many alkylcyclohexenes undergo reversible isomerization to alkylcyclopentenes. In some cases the isomerization consists of shift of the double bond without ring contraction. Side reactions, in this case, involve hydrogen transfer (disproportionation) to yield cycloalkanes and aromatics. In the presence of activated alumina cyclohexene is converted to a mixture of 1-methyl- and 3-methyl-1-cyclopentene 103... 

Rhodium(II) acetate catalyzes C—H insertion, olefin addition, heteroatom-H insertion, and ylide formation of a-diazocarbonyls via a rhodium carbenoid species (144—147). Intramolecular cyclopentane formation via C—H insertion occurs with retention of stereochemistry (143). Chiral rhodium (TT) carboxamides catalyze enantioselective cyclopropanation and intramolecular C—N insertions of CC-diazoketones (148). Other reactions catalyzed by rhodium complexes include double-bond migration (140), hydrogenation of aromatic aldehydes and ketones to hydrocarbons (150), homologation of esters (151), carbonylation of formaldehyde (152) and amines (140), reductive carbonylation of dimethyl ether or methyl acetate to 1,1-diacetoxy ethane (153), decarbonylation of aldehydes (140), water gas shift reaction (69,154), C—C skeletal rearrangements (132,140), oxidation of olefins to ketones (155) and aldehydes (156), and oxidation of substituted anthracenes to anthraquinones (157). Rhodium-catalyzed hydrosilation of olefins, alkynes, carbonyls, alcohols, and imines is facile and may also be accomplished enantioselectively (140). Rhodium complexes are moderately active alkene and alkyne polymerization catalysts (140). In some cases polymer-supported versions of homogeneous rhodium catalysts have improved activity, compared to their homogenous counterparts. This is the case for the conversion of alkenes direcdy to alcohols under oxo conditions by rhodium—amine polymer catalysts... 

Nitriles. The molecular ion peak is weak or non-existent in aliphatic nitriles but strong in aromatic compounds. Interpretation of the spectrum is often difficult since skeletal rearrangements are common and the resulting ion series (m/z 41, 55, 69, etc.) overlaps with that arising from hydrocarbons. Thus in the McLafferty rearrangement ... 

Among all the isotetracene antibiotics, tetrangomycin (32a), obtained from S. rimosus, possesses the simplest structure, and is the first antibiotic to be isolated [162, 163]. Compound (32a) differs from (31) only by the presence of a double bond (instead of a diol) between C-4a and C-12b. Base treatment of (32a) does not cause a skeletal rearrangement, but readily aromatizes it to the benz[a]anthraquinone derivative, tetrangulol (33a). The latter is an antibiotic per se, since it can also be isolated from the culture filtrates of S. rimosus without any alkaline treatment [162]. A related antibiotic rabelomycin (32b)... 

Skeletal rearrangement reactions over Pt single crystals have been studied for methyl cyclopentane, 2- and 3-methylpentane350 and for n-hexane.3sl One conclusion351 is that whereas aromatization reactions are very sensitive to surface structure [Pt(l 11)> Pt(100)], isomerization, Cs-cyclization, and hydrogenolysis reactions display little dependence on structure. Temperature and H2 pressure are more important in affecting the selectivity. 

Surprisingly, gold can also catalyze skeletal rearrangements of hydrocarbons for instance, the isomerization of 2,2-dimethylbutane to n-hexane has been achieved by Schmid with the aid of AU55 clusters on titanium dioxide [4c, 6] and the aromatization of the dispirocycle 1 to tetrahydronaphthalene 2 was achieved by de Meijere et al. in a reactor with gold surface at 100 °C in a few seconds (Scheme 1) [7]. 

Muller, M., Iyer, V.S., Ktibel, C., Enkelmann, V. and Mullen, K. (1997) Polycyclic aromatic hydrocarbons by cyclodehydrogenation and skeletal rearrangement of oligophenylenes. Angewandte Chemie (International Ed. in English), 36,1607-10. 

Oxetanes have also been used as alkylating agents in the Friedel-Crafts reaction for example, 2-isopropyloxetane was reacted with benzene in superacidic trifluoromethanesulfonic acid (TFSA) to give a mixture of alkylated aromatic products (Equation 9) <2003CAL1>. The main product of the reaction was the tetralin derivative 46 which could be isolated in up to 75% yield. Other notable side products are shown, resulting from monoalkylation or other skeletal rearrangements. 

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