Oxidation acyclic

Dimethyldioxirane oxidizes acyclic vinylsilanes at room temperature to the corresponding epoxides 166 in excellent yield (equation 141)255. Allylic oxidation is found in appreciable amounts when cyclic vinylsilanes are used. It is interesting to note that simple alkenes react faster with dioxirane than vinylsilanes. The trend appears to be reversed when MCPBA is employed as the oxidant. 

In 1966, it was found that stoichiometric amounts of Fe203 were capable of oxidizing acyclic thiols to disulfides in hydrocarbon media at 55 °C (Scheme 3.47) [149]. 

With the powerful formylation reagent IV -diformylacetamide imides are obtained from amides or lactams in good yield (equation 56). Oxidation reactions also have found some application in the synthesis of imides. For example, catalytic amounts of ruthenium tetroxide and 10% aqueous NaI04 as cooxidant in an optimized reaction medium (ethyl acetate-water) oxidize acyclic amides to imides. The reaction rate is inversely related to the electron-withdrawing power of the acyl group, i.e. the electron density at the nitrogen atom (equation 57). 

Oxidations. Dimethyl selenoxide is more effective than dimethyl sulfoxide (4,194 6, 227) for oxidation of trivalent phosphorus and thiocarbonyl compounds. It oxidizes acyclic P(III) compounds to oxides (with nearly complete inversion of configuration) cyclic P(III) compounds are oxidized with retention of configuration. The same stereochemical result obtains in oxidations with DMSO. 

Recent syntheses of steroids apply efficient strategies in which open-chain or monocyclic educts with appropiate side-chains are stereoselectively cyclized in one step to a tri- or tetracyclic steroid precursor. These procedures mimic the biochemical synthesis scheme where acyclic, achiral squalene is first oxidized to a 2,3-epoxide containing one chiral carbon atom and then enzymatically cyclized to lanostetol with no less than seven asymmetric centres (W.S. Johnson, 1%8, 1976 E.E. van Tamden, 1968). 

Stereochemical features in the oxidative addition and the elimination of /3-hydrogen of cyclic and acyclic alkenes are different. The insertion (palladation) is syn addition. The syn addition (carbopalladation) of R—Pd—X to an acyclic alkene is followed by the syn elimination of 3-hydrogen to give the trans-a ksne 6, because free rotation of 5 is possible with the acyclic alkene. On the other hand, no rotation of the intermediate 7 is possible with a cyclic alkene and the syn elimination of /3-hydrogen gives the allylic compound 8 rather than a substituted alkene. 

Conversion of Cyclic to Acyclic Structures. Upon oxidation, the aromatic rings of lignin may be converted direcdy to acycHc stmctures, eg, muconic acid derivatives, or indirectly by oxidative splitting of o-quinoid rings. Further oxidation creates carboxyUc acid fragments attached to the lignin network. 

A variety of 1-azirines are available (40-90%) from the thermally induced extrusion (>100 °C) of triphenylphosphine oxide from oxazaphospholines (388) (or their acyclic betaine equivalents), which are accessible through 1,3-dipolar cycloaddition of nitrile oxides (389) to alkylidenephosphoranes (390) (66AG(E)1039). Frequently, the isomeric ketenimines (391) are isolated as by-products. The presence of electron withdrawing functionality in either or both of the addition components can influence the course of the reaction. For example, addition of benzonitrile oxide to the phosphorane ester (390 = C02Et) at... 

Electron deficient carbon-carbon double bonds are resistant to attack by the electrophilic reagents of Section 5.05.4.2.2(t), and are usually converted to oxiranes by nucleophilic oxidants. The most widely used of these is the hydroperoxide ion (Scheme 79). Since epoxidation by hydroperoxide ion proceeds through an intermediate ct-carbonyl anion, the reaction of acyclic alkenes is not necessarily stereospecific (Scheme 80) (unlike the case of epoxidation with electrophilic agents (Section 5.05.4.2.2(f)) the stereochemical aspects of this and other epoxidations are reviewed at length in (B-73MI50500)). 

Diazoalkanes add to the carbon-carbon double bonds of 2,3-diphenylthiirene 1-oxide and 1,1-dioxide. The adducts lose SO or SO2 to give pyrazoles and related compounds (Scheme 103) (80CB1632). Mesoionic oxazolones (75CLH53), 4-methyl-5-phenyl-l,2-dithiolene-3-thione (80JOU395) and pyrylium betaines (72JOC3838) react similarly via intermediate adducts (Scheme 104). Enamines (Scheme 96) and ynamines add to the double bond of 2,3-diarylthiirene 1,1-dioxides to give acyclic and cyclic sulfones by a thermal. 

A carbonyl group can be protected as a sulfur derivative—for example, a dithio acetal or ketal, 1,3-dithiane, or 1,3-dithiolane—by reaction of the carbonyl compound in the presence of an acid catalyst with a thiol or dithiol. The derivatives are in general cleaved by reaction with Hg(II) salts or oxidation acidic hydrolysis is unsatisfactory. The acyclic derivatives are formed and hydrolyzed much more readily than their cyclic counterparts. Representative examples of formation and cleavage are shown below. 

The accessibility of the +4 and +6 oxidation states for sulfur and, to a lesser extent, selenium gives rise to both acyclic and cyclic molecules that have no parallels in N-O chemistry. Thus there is an extensive chemistry of chalcogen diimides RN=E=NR (E = S, Se, Te) (Section 10.4). In the case of Te these unsaturated molecules form dimeric structures reflecting the increasing reluctance for the heavier chalcogens to form multiple bonds to nitrogen. The acyclic molecule N=Sp3,... 

The interesting tautomeric equilibrium 299 300 has not yet been reported for heterocyclic A -oxides, although it has been described for acyclic compounds. ... 

Occasionally it happens that the oxo compound, produced by oxidation, forms a hydrate which is further oxidized to a dihydroxy compound. Attention must be given to the possibility (so far unreported) that when the hydrated species is in equilibrium with a trace of the ring-opened structure a sufficiently fast oxidation rate of the amino-aldehyde (i.e. the acyclic structure) could lead to the incorrect conclusion that the original material was not cyclic. 

For the construction of oxygen-functionalized Diels-Alder products, Narasaka and coworkers employed the 3-borylpropenoic acid derivative in place of 3-(3-acet-oxypropenoyl)oxazolidinone, which is a poor dienophile in the chiral titanium-catalyzed reaction (Scheme 1.55, Table 1.24). 3-(3-Borylpropenoyl)oxazolidinones react smoothly with acyclic dienes to give the cycloadducts in high optical purity [43]. The boryl group was converted to an hydroxyl group stereospecifically by oxidation, and the alcohol obtained was used as the key intermediate in a total synthesis of (-i-)-paniculide A [44] (Scheme 1.56). 

Acylation of norephedrine (56) with the acid chloride from benzoylglycolic acid leads to the amide (57), Reduction with lithium aluminum hydride serves both to reduce the amide to the amine and to remove the protecting group by reduction (58), Cyclization by means of sulfuric acid (probably via the benzylic carbonium ion) affords phenmetrazine (59), In a related process, alkylation of ephedrine itself (60) with ethylene oxide gives the diol, 61, (The secondary nature of the amine in 60 eliminates the complication of dialkylation and thus the need to go through the amide.) Cyclization as above affords phendimetra-zine (62), - Both these agents show activity related to the parent acyclic molecule that is, the agents are CNS stimulants... 

Recently, solicon-tethered thastereoselecdve ISOC reactions have been reported, in which effective control of remote acyclic asymmetry can be achieved fEq 8 91) Whereas ISOC occur stereoselecdvely, INOC proceeds v/ith significandy lower levels of diastereoselecdon The reaction pathways presented in Scheme 8 28 suggest a plausible hypothesis for the observed difference of stereocontrol The enhanced selecdvity in reacdons of silyl nitronates may be due to l,3- illylic strain The near-linear geometry of nitnle oxides precludes such differendadng elements fScheme 8 28 ... 

The oxidation of active methylene groups by periodate both in acyclic... 

The C2-symmetric epoxide 23 (Scheme 7) reacts smoothly with carbon nucleophiles. For example, treatment of 23 with lithium dimethylcuprate proceeds with inversion of configuration, resulting in the formation of alcohol 28. An important consequence of the C2 symmetry of 23 is that the attack of the organometallic reagent upon either one of the two epoxide carbons produces the same product. After simultaneous hydrogenolysis of the two benzyl ethers in 28, protection of the 1,2-diol as an acetonide ring can be easily achieved by the use of 2,2-dimethoxypropane and camphor-sulfonic acid (CSA). It is necessary to briefly expose the crude product from the latter reaction to methanol and CSA so that the mixed acyclic ketal can be cleaved (see 29—>30). Oxidation of alcohol 30 with pyridinium chlorochromate (PCC) provides alde-... 

Without question, the most significant advance in the use of sulfur-centered nucleophiles was made by Shibasaki, who discovered that 10 mol% of a novel gallium-lithium-bis(binaphthoxide) complex 5 could catalyze the addition of tert-butylthiol to various cyclic and acyclic meso-epoxides with excellent enantioselectiv-ities and in good yields (Scheme 7.11) [21], This work builds on Shibasaki s broader studies of heterobimetallic complexes, in which dual activation of both the electrophile and the nucleophile is invoked [22]. This method has been applied to an efficient asymmetric synthesis of the prostaglandin core through an oxidation/ elimination sequence (Scheme 7.12). 

Nakajima reported the use of a chiral bipyridine N,N -dioxide 18 in the desym-metrization of acyclic meso epoxides (Figure 7.3). Although the enantioselectivity was not as high as in the method developed by Fu for meso-stilbene oxide (90% ee vs. 94% ee), it was higher for the same aliphatic epoxide (74% ee vs. 50% ee) [57]. Nakajima showed that mono-N-oxide derivatives 19 and 20 were much less effective than 18 in tenns of both yield and enantioselectivity, and accordingly proposed a unique mechanism for 18 involving a hexacoordinate silicon intermediate coordinated to both N-oxides of the catalyst. 

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