Isoxazoline compounds

Stojanovic, I., Cuzzocrea, S., Mangano, K., Mazzon, E., Miljkovic, D., Wang, M., Donia, M., A1 Abed, Y., Kim, J., Nicoletti, F., Stosic-Gmjicic, S., and Claesson. M. (2007). In vitro, ex vivo and in vivo iimnunopharmacological activities of the isoxazoline compound VGX-1027 modulation of cytokine synthesis and prevention of both organ-specific and systemic autoinunune diseases in murine models. Clin. Immunol. 123, 311-323. 

Pyrroles from 1,4-dicarbonyl compounds and ammonia isoxazolines from olefins and nitrile oxides. 

Diacetates of 1,4-butenediol derivatives are useful for double allylation to give cyclic compounds. l,4-Diacetoxy-2-butene (126) reacts with the cyclohexanone enamine 125 to give bicyclo[4.3.1]decenone (127) and vinylbicy-clo[3.2.1]octanone (128)[85,86]. The reaction of the 3-ketoglutarate 130 with cij-cyclopentene-3,5-diacetate (129) affords the furan derivative 131 [87]. The C- and 0-allylations of ambident lithium [(phenylsulfonyl)methylene]nitronate (132) with 129 give isoxazoline-2-oxide 133, which is converted into c -3-hydroxy-4-cyanocyclopentene (134)[S8]. Similarly, chiral m-3-amino-4-hyd-roxycyclopentene was prepared by the cyclization of yV-tosylcarbamate[89]. 

Dimethylsulfonium phenacylide (574) underwent C-alkylation with a-chloronitroso compounds such as (575). The intermediate (576) immediately cyclized to the isoxazoline (577). With a more basic ylide such as dimethylsulfonium methoxycarbonylmethylide the initial alkylation product underwent elimination of the sulfonium group to an alkene rather than its displacement (72T3845). 

The photolysis of 4-substituted 2,3-dimethyl-3-isoxazolin-5-ones has been studied. Irradiation in methanol or ethanol with a 100 W high-pressure mercury lamp through a Pyrex filter of a 4-phenylthio compound produced a semithioacetal (Scheme 5). In contrast, an H, Cl or OPh moiety gave no reaction. The use of alkylthio substitution gave similar products. Cyclic compounds yielded cyclic products (Scheme 5), and the photolysis of (29) in benzene... 

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). 

When compound (443), which contains alkene and alkyne moieties, was reacted with benzonitrile oxide, both an isoxazoline (444) and isoxazole (445) were produced, with the former predominating. Oxidation of (444) with permanganate produced 3-phenyl-2-isoxazoline-5-carboxylic acid (446) (67ZOR82i). The reaction of 1-trimethylsilylbut-l-yne-3-ene produced only a compound which reacted at the alkenic unit. Oxidation of the adduct also produced (446) (68ZOB1820). These reactions are shown in Scheme 102. 

The cycloaddition of benzonitrile oxide to cis- and rrans-l,2-dichloroethylene produced the appropriate cis- and trans-4,5-dichloro-3-phenyl-2-isoxazoline diastereomers. Base elimination produced only one compound, 4-chloro-3-phenyloxazole (Scheme 103) (70CJC3753). 

The reaction of arylnitrile oxides with 1,1-diphenylallenes gave a mixture of 4-methylene-2-isoxazolines (Scheme 106) with major attack at the C(2)—C(3) double bond (74JCS(P2)l30l, 76CSC67, 76CSC71, 72JCS(P2)1914) and not a mixture of the 4- and 5-methylene compounds. 1-Phenoxyallene and benzonitrile oxide produced a mixture of positional isomers and a spiro compound (Scheme 107) (79JOC2796). 

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 reaction of a dibromochalcone with hydroxylamine hydrochloride in pyridine gave three products with the expected 2-isoxazoline product as the predominate compound. A ring bromination product and an isoxazole were also isolated (70UC796). The reaction of hydroxylamine with /S-thiosulfates of propiophenone at reflux produced 3-phenyl-2-isoxazo-line (455). At room temperature a bis-Michael product (456) was produced. The reaction with N -phenylhydroxylamine yielded a mono-Michael type product (457) (74CPB1990). 

Alkylnitro compounds when treated with acetic anhydride and triethylamine produced furoxans. With an alkene present, 2-isoxazolines are isolated (Scheme 120) (78MI41610). 

This small class of compounds is characterized by an N-alkyl moiety, and they are synthesized from isoxazolium salts by isomerization or by the dehydration of 2-alkyl-isoxazolidin-3-ols (Scheme 128) (74BSF1025). The reaction of isoxazolium salts that are unsubstituted in the 5-position with phenylmagnesium halides was reported to give 3-isoxazolines by 1,4-conjugate addition, and this reaction is also shown in Scheme 128 (74CPB70). 

Bravo et al. studied the reaction of various ylides with monooximes of biacetyl and benzil. Dimethylsulfonium methylide and triphenylarsonium methylide gave 2-isoxazolin-5-ol and isoxazoles, with the former being the major product. Triphenylphosphonium methylide and dimethyloxosulfonium methylide gave open-chain products (Scheme 135) (70TL3223, 72G395). The cycloaddition of benzonitrile oxide to enolic compounds produced 5-ethers which could be cleaved or dehydrated (Scheme 136) (70CJC467, 72NKK1452). 

Haloisoxazolium salts were treated with Na2S to produce the above titled compounds (76ZC270). For example, 5-chloro-2-methyl-3-phenylisoxazolium tetrafluoroborate and Na2S gave 2-methyl-3-phenyl-3-isoxazoline-5-thione. 

This series of compounds was also discussed briefly by Quilico in 1962 and only a limited number of new representatives have been reported 62HC(17)l,p. 3). The pressure reaction of ethylene and nitric acid in the presence of Ni, Zn or Cu produced 3,3 -bis(isoxazoline) 70FRP94493), and the isoxazoline IV-oxide (515) was prepared by the reaction of /3-dimethylaminoacrylaldehyde and methyl nitroacetate (74IZV845). 

This system was generated by the reaction of hydroxylamine with malonyl dihalides (65HCA1973, 80AP39) Or by the saponification of 3-isoxazolin-5-ones as shown in Scheme 163. These compounds are strong acids and can exist in a variety of forms, with the dione form being the most favored (equation 58) (80JHC299). 

Reaction of 2-(A -allylamino)-3-formyl-4//-pyrido[l, 2-u]pyrimidin-4-ones 219 in EtOH with HONH2 HCI yielded ( )-oximes 220 at 0°C and 221 (R = PhCH2) under reflux. Heating 220 (R = H) in a boiling solvent afforded cw-fused tetracyclic cycloadducts 221 (R = H). In an aprotic solvent (e.g., benzene or MeCN) the main a>fused cycloadducts 221 (R = H) were accompanied by a mixture of trauA-fused cycloadducts 222, A -oxides 223 and tetracyclic isoxazoline 224 (96T887). The basicity of the 2-allylamino moiety of compounds 219 affected the rate of the conversion. Cycloadditions were also investigated in dioxane and BuOH. 

One of the most important routes to isoxazole and isoxazoline rings involving the formation of the 1—5 and 2—3 bonds involves the condensation of hydroxylamine with a,/8-unsaturated carbonyl compounds. This method was previously widely used, but it is now of no preparative value, though it has been recently applied to determine the configuration of oximes. " The only new modification of this synthesis is the use of the acetals (27) of a,/8-acetylenic aldehydes for preparation of 5-substituted isoxazoles (28)... 

As already mentioned, on passing from the aromatic system of isoxazoles to the nonaromatic ones of isoxazolines and isoxazolidines, the N—O bond becomes more labile. In these compounds the ring is extremely readily cleaved. Many such reactions are useful to determine the structure of reduced isoxazole derivatives and are also of preparative value. 

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. 

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