Amino-oxazolines

Other chiral grafting species which were linked to mesoporous pure silica phases in order to study chiral catalysis reactions include alkaloids and alkaloid derivates (cinchona and ephedrine ), bis(oxazoline), amino alcohols, proline... 

Keywords Amino-oxazolines Amino-thiazolines Nucleosides Oxazolidine-2-thiones Sugar isothiocyanates Thiocarbamates... 

These oxazolines have cationic surface-active properties and are emulsifying agents of the water-in-oil type. They ate acid acceptors and, in some cases, corrosion inhibitors (see Corrosion). Reaction to oxazoline also is useful as a tool for determination of double-bond location in fatty acids (2), or for use as a protective group in synthesis (3). The oxazolines from AEPD and TRIS AMINO contain hydroxyl groups that can be esterified easily, giving waxes (qv) with saturated acids and drying oils (qv) with unsaturated acids. 

Formaldehyde reacts with the hydrogen on the a-carbon of the fatty acid from which the oxazoline was formed to yield a vinyl monomer which can be polymerized or utilized for synthesis (4). Thus, esters of the oxazoline formed from TRIS AMINO undergo the reaction... 

Synthetic Applications. Oxazolines, which ate synthesized as indicated above, have been utilized in many different appHcations (25). When used in resin formulations, AMP, AEPD, and TRIS AMINO can incorporate the oxazoline stmeture into the polymer stmeture (26). Because they ate polyols, both AEPD and TRIS AMINO can be used in polyester resin modification. Oxazoline alkyd films ate characterized by improved performance, particularly salt-spray resistance and gloss (see Alkyd resins Coatings, special purpose, high performance). 

Ring fission occurs readily in many of these compounds. For example, azlactones, i.e. 4JT-oxazolin-5-ones containing an exocyclic C=C bond at the 4-position (508), are hydrolyzed to a-benzamido-a,/3-unsaturated acids (509), further hydrolysis of which gives a-keto acids (510). Reduction and subsequent hydrolysis in situ of azlactones is used in the synthesis of a-amino acids e.g. 508 -> 507). 

A number of 2-acylazetidines have been prepared by reaction of 1,3-dihaloacyl compounds with amino derivatives (Section 5.09.2.3.l(m)). This is illustrated for azetidine 2-carboxylic acid (56), the only known naturally occurring azetidine. Ring expansion of activated aziridines (43) and contraction of 4-oxazolines (55) has also found limited use (Section 5.09.2.3.2(f) and Hi)). 

The first synthesis and use of a chiral oxazoline was reported by Meyers in 1974. The chiral oxazoline 1 was prepared in two steps by condensation of (-i-)-l-phenyl-2-amino-1,3-propanediol (6) with the ethyl imidate of propionitrile followed by 0-methylation of the resulting alcohol 7 with NaH/Mel. Meyers demonstrated chiral oxazoline 1 could be... 

P-amino acid products. Treatment of oxazoline 53 with 7V-lithiopiperidine followed by alkylation with iodomethane affords aniline derivative 54 in 94% yield and 99% de. Hydrolysis of the oxazoline group provided amino acid 55 in 92% yield and >99% ee. 

More recent examples have employed a milder reagent system, triphenyl-phosphine and dibromotetrachloroethane to generate a bromo-oxazoline, which is subsequently dehydrohalogenated. Wipf and Lim utilized their method to transform intermediate 11 into the 2,4-disubstituted system of (+)-Hennoxazole k Subsequently, Morwick and coworkers reported a generalized approach to 2,4-disubstituted oxazoles from amino acids using a similar reagent combination, triphenylphosphine and hexachloroethane. ... 

With 1,2-diaminoethane or 1-amino-2-hydroxyethane, for example, 4-dialkyl-aminobut-3-yn-2-ones react in THF solution at 65-70°C without catalyst (2 h) to form the corresponding 2-(acetylmethyl)-1,3-imidazolines (346) (70% yield) and 2-(acetylmethyl)-l,3-oxazolines (347) (61% yield), respectively (88USSRP1330133 88ZOR1165). 

Aminoenyne ketones 350 (90ZOR2508) react with 1,2-diaminoethane and 1-amino-2-hydroxyethane analogously as a twofold nucleophilic attack at the triple bond followed by elimination of diethylamine to afford imidazolines 351 and oxazolines 352, which also contain a strong hydrogen bond and a completely enolyzed vinylacetyl group (92KGS1409 94ZOR51). 

Investigation- of oxazoline derivatives using infrared spectroscopy and pK measurements showed that the amino forms 178 and 179... 

In this aforementioned Heine reaction the initial ring opening takes place by iodide ions. Subsequent ring closure by S 2 displacement of iodide by reaction with the negative oxygen center then leads to the products. This process proceeds with double inversion at the same carbon atom, thus with net retention. Hydrolysis of these oxazolines gives j9-hydroxy-a-amino acids (Scheme 31) [1,38]. The stereochemical course of ring expansion is the same as that observed in Scheme 29. 

Fujisawa et al. [Ill] have reported that the magnesiiun complex prepared from chiral 2-[2-[(tolylsulfonyl)amino]phenyl]-4-phenyl-l,3-oxazoline 81 and methyl-magnesium iodide was efficient, in a stoechiometric amount, for promoting the enantioselective Diels-Alder reaction of 3-alkenoyl-l,3-oxazohdin-2-one with cyclopentadiene (Scheme 45) leading exclusively to the endo adducts in up to 92% ee. The use of 10 mol% of the complex led to an important decrease in enantioselectivity of the product (51% ee). 

The more difficult problem of protecting the carbonyl group can be accomplished by conversion to a oxazoline derivative. One example is the 4,4-dimethyl derivative, which can be prepared from the acid by reaction with 2-amino-2-methylpropanol or with 2,2-dimethylaziridine.269... 

It is worth mentioning here that the spirocyclopropyl-substituted oxazoline-5-car-boxylates 2-172, as well as the corresponding thiazoline-4-carboxylates, can be transformed into cyclopropyl-substituted amino acids, which might act as potential enzyme inhibitors [93] and interesting building blocks for peptidomimetics [94]. 

Helmchen and coworkers employed a,co-amino-1,3-dienes as substrates [51]. By using palladium complexes with chiral phosphino-oxazolines L as catalysts, an enantiomeric excess of up to 80 % was achieved. In a typical experiment, a suspension of Pd(OAc)2, the chiral ligand L, the aminodiene 6/1-90 and an aryltriflate in dimethylformamide (DMF) was heated at 100 °C for 10 days. Via the chiral palladium complex 6/1-91, the resulting cyclic amine derivative 6/1-92 was obtained in 47% yield and 80% ee (Scheme 6/1.23). Using aryliodides the reaction time is shorter, and the yield higher (61 %), but the enantiomeric excess is lower (67% ee). With BINAP as a chiral ligand for the Pd°-catalyzed transformation of 6/1-90 and aryliodide, an ee-value of only 12% was obtained. 

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