Isoxazolines nitro compounds

The two major methods of preparation are the cycloaddition of nitrile oxides to alkenes and the reaction of a,/3-unsaturated ketones with hydroxylamines. Additional methods include reaction of /3-haloketones and hydroxylamine, the reaction of ylides with nitrile oxides by activation of alkyl nitro compounds from isoxazoline AT-oxides (methoxides, etc.) and miscellaneous syntheses (62HC(i7)i). 

The reaction of alkyl nitro compounds with acetyl chloride in the presence of an alkenic compound produced a 2-isoxazoline. The mechanism is believed to proceed via a nitrile oxide and is illustrated in Scheme 112 (B-79MI41613). 

The base-catalysed reaction of a-bromo-a,P-unsaturated ketones with aliphatic nitro compounds leads to 2-isoxazoline A-oxides by tandem conjugate addition-ring closure (Scheme 5) <95JOC6624>. A -Acyl-3-isoxazolin-5-ones are transformed into oxazoles by photolysis or by flash vacuum pyrolysis (Scheme 6) <96TL675>. 

Monoalkylation of Af-tosylallylamine 10 with dibromoalkane 101 proceeded in 60-90% yield (Eq. 10 see also Scheme 3 and Eq. 2) [17]. The bromoalkyl-amines 102 were converted to nitro compounds 103. In situ transformation of 103 into nitrile oxides led to spontaneous cycloaddition with formation of isox-azolines fused to 5-, 6-, and 7-membered ring heterocycles 104 a-c. Under very high dilution conditions, 103 d was converted to 104 d, an isoxazoline fused to an 8-membered azocine, in low (10%) yield. 

Primary nitro compounds are good precursors for preparing nitriles and nitrile oxides (Eq. 6.31). The conversion of nitro compounds into nitrile oxides affords an important tool for the synthesis of complex natural products. Nitrile oxides are reactive 1,3-dipoles that form isoxazolines or isoxazoles by the reaction with alkenes or alky nes, respectively. The products are also important precursors for various substrates such as P-amino alcohols, P-hydroxy ketones, P-hydroxy nitriles, and P-hydroxy acids (Scheme 6.3). Many good reviews concerning nitrile oxides in organic synthesis exist some of them are listed here.50-56 Applications of organic synthesis using nitrile oxides are discussed in Section 8.2.2. 

As discussed in Section 6.2, nitro compounds are good precursors of nitrile oxides, which are important dipoles in cycloadditions. The 1,3-dipolar cycloaddition of nitrile oxides with alkenes or alkynes provides a straightforward access to 2-isoxazolines or isoxazoles, respectively. A number of ring-cleaving procedures are applicable, such that various types of compounds may be obtained from the primary adducts (Scheme 8.18). There are many reports on synthetic applications of this reaction. The methods for generation of nitrile oxides and their reactions are discussed in Section 6.2. Recent synthetic applications and asymmetric synthesis using 1,3-dipolar cycloaddition of nitrile oxides are summarized in this section. 

Nitro compounds have also been reported to undergo photocyclizations. The intermediacy of an isoxazoline in the photorearrangement of o-nitro-benzaldehyde to o-nitrosobenzoic acid is now in doubt,318 but intramolecular hydrogen abstraction by an excited nitro group in nitrobenzene derivatives can result in the formation of heterocycles. 4-tm-Butyl-3-methoxy-2,6-dinitrotoluene (384) on irradiation in methanolic sodium hydroxide solution... 

A detailed study of the role of the base in the formation of 2-isoxazolines by condensation of primary nitro compounds with alkenes in the presence of the tertiary diamine 1,4-diazabicyclo[2.2.2]octane (DABCO) was published <06EJO4852 06EJ03016>. 

Isoxazolines A-oxides have been synthesized from primary aliphatic nitro compounds and alkenes by a two-step procedure consisting of 1,3-DC of a 1-halo-substituted silyl nitronate followed by halosilane elimination <06S2265>. 

From the 1980s on, many efforts were directed toward asymmetric induction of nitrile oxide cycloadditions to give pure (dia)stereoisomeric isoxazolines, and acyclic products derived from them (17,18,20-23). The need to obtain optically active cycloaddition products for use in the synthesis of natural products was first served by using chiral olefins, relying on 1,2-asymmetric induction, and then with optically active aldehydes or nitro compounds for the nitrile oxide part. In the latter case, insufficient induction occurs using chiral nitrile oxides, a problem still unsolved today. Finally, in the last 5 years, the first cases of successful asymmetric catalysis were found (29), which will certainly constitute a major area of study in the coming decade. 

Intramolecular cycloadditions of alkenyl-substituted nitrile oxides produce bicyclic isoxazolines. When monocyclic olehns are used, tricyclic structures are obtained. This approach was pioneered by both Kozikowski s and Curran s groups. A typical case involves the cycloaddition of nitro compound 191 [mixture of diastereomers derived from pentenose pyranoside 190], which produced a diaster-eomeric mixture of isoxazolines that contain cis-fused rings (i.e., 192) in near quantitative yield (326) (Scheme 6.85). Further elaboration of this mixture led to epoxycyclopentano-isoxazoline 193, which was then converted to the aldol product in the usual manner. The hydrogenation proceeded well only when rhodium on alumina was used as the catalyst, giving the required p-hydroxyketone 194. This... 

An intramolecular cycloaddition of the tetradecatrienyl nitroethyl ether 263 was used in the synthesis of the 14-membered bicyclic precursor 265 of crassin acetate 266, a cembrane lactone possessing antibiotic and antineoplastic activity (332). Nitro compound 263 was obtained from farnesyl acetate (262) in several steps and was then treated with phenyl isocyanate and triethylamine to give the tricyclic isoxazoline 264 (Scheme 6.98). Conversion to ketone 265 was accomplished by hydrogenation of the cycloadduct with Raney Ni and boric acid followed by acetylation (332). In this case, the isoxazoline derived from a 3-butenyl nitroethyl ether moiety served to produce a 3-methylenetetrahydropyran moiety (332). 

One of the very first uses of the intramolecular nitrile oxide cycloaddition involved the synthesis of macrocyclic lactones. Asaoka et al. (238) conceived this approach to the 16-membered ring antibiotic A26771B (277). Nitro compound 274 [obtained from 11-acetoxydodecanal (273)] was dehydrated with 4-chlorophenyl isocyanate-triethylamine and this was followed by dipolar cycloaddition, which gave isoxazoline 275 as a 4 1 mixture of diastereomers (Scheme 6.100). 

Aliphatic nitro compounds are versatile building blocks and intermediates in organic synthesis,14 15 cf. the overview given in the Organic Syntheses preparation of nitroacetaldehyde diethyl acetal.16 For example, Henry and Michael additions, respectively, lead to 1,2- and 1,4-difunctionalized derivatives.14 18 1,3-Difunctional compounds, such as amino alcohols or aldols are accessible from primary nitroalkanes by dehydration/1,3-dipolar nitrile oxide cycloaddition with olefins (Mukaiyama reaction),19 followed by ring cleavage of intermediate isoxazolines by reduction or reduction/hydrolysis.20 21... 

Macro carbocyclic rings can be constructed by cyclization of nitrile oxides derived from oj-nitro-l-al-kenes (Scheme 22). If the intervening bridge is not longer than seven atoms, only fused bicyclic products are obtained. Thus, the nitrile oxide derived from nitro compound (75a) is cyclized in 44% yield to the 5,9-fused bicyclic isoxazoline (76a).38 10-Nitro-l-decene (75b) also cyclized to (76b) in unspecified yield.39 It should be noted that these results go counter to the usual regiochemistry of an intermolecular nitrile oxide cycloaddition where the five-substituted isoxazoline is usually,27 although not always,40 heavily preferred from reaction of a terminal alkene. Thus, geometric constraints have won out over the normal electronic control. 

Secondary amines can be oxidized at the N-H bond to hydroxylamines and nitroxides, and via nitrones via C-N oxidation. Nitrones are valuable intermediates in the production of isoxazolines. Initial C-N oxidation of secondary amines gives imines which can react further to oxaziridines. The latter can be converted to nitrones, and both to amides. Primary amines are oxidized at the N-H bond to mono-substituted hydroxylamines, which are readily converted further to nitroso and nitro compounds by the more activated peroxygen... 

From the parent nitro compound -PrN02 (68), formal elimination of one water molecule with phenyl isocyanate gives the desired nitrile oxide 69 (the 1,3-dipole), aniline and CO2. Then, an isoxazoline is made by cycloaddition of 69 with the terminal olefin of the substrate (dipolarophile). ... 

Isoxazolines and isoxazolidines, synthesis from aliphatic nitro compounds... 

Polymer-supported enzymes have been combined with polymer-supported reagents in the synthesis of the bryostatins. The nitrone derived from the nitro compound 43 supported on a soluble aryl poly-ether polymer undergoes an efficient 1,3-dipolar cycloaddition with butenone to give the isoxazoline 44 and hence by reduction the racemic syn compound 45 required for the synthesis.16... 

Nitrile oxides (R-C=N -0 ), which can be generated by base-catalysed ehmination of hydrogen halide from halooximes (RC(Hal) = NOH), or by dehydration of nitro compounds" (RCH2NO2), readily add to alkenes and to alkynes generating five-membered heterocycles. Addition to an alkene produces an isoxazo-line, unless the alkene also incorporates a group capable of being eliminated in a step after the cycloaddition as shown below isoxazolines can be dehydrogenated to the aromatic system. 

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