Ring kinetics

Benzyne was shown to react with a variety of monocyclic and fused-ring thiiranes to produce vinyl thiophenyl ethers <84TL2679>. Initial reaction gives an intermediate betaine, which abstracts the most acidic (kinetic) ring proton, with concomitant C=C bond formation and C—S bond scission, to give excellent yields of products (illustrated for (2) in Scheme 3). The stereochemistry of the starting thiiranes is preserved in the product vinyl sulfides. 

We have shown in the previous sections that in certain systems (e.g. polymerization of cyclic formals studied by Schulz 7 8) and Y amashita 20>) one can use kinetic enhancement to obtain higher proportions of macrocyclics. This is mostly due to the enhanced contribution of the end-to-end closure. There are systems (THF2- 3), cyclic sulfides 25y) in which kinetic ring-depression was observed due to a slow rate of cyclization and thus the equilibrium concentration of the rings was attained only slowly. These two extreme cases are depicted in Fig. 3.9. 

M. Newcomb, C. C. Johnson, M. D. Manek, and T. R. Varick. Picosecond radical kinetics. Ring openings of phenyl-substituted cyclopropylcarbinyl radicals. J. Am. Chem. Soc., 114 10915 (1992). 

Summarizing the kinetic ring-opening polymerizability/ reactivity it should be stressed that there are a larger number of monomers polymerizing cationically than anionically. This can be understood when the cationic and anionic propagation steps are compared ... 

The kinetics of this type of polymerization are the same as for simple condensation for this reason, the use of the term polycondensation is perhaps more appropriate. Unless kinetic evidence suggests otherwise, polymerizations involving the formation of chain polymers from cyclic compounds, following ring scission, are classed as condensation polymerizations. Some important con-... 

For irreversible ring closure reaction, the kinetic product will predominate. 

The nitration of phenylpyridines and related compounds has attracted attention for a long time, and measurements of isomer proportions have been made for several compounds of this type. Nitration occurs in the phenyl ring. For 2-phenylpyridine and 2-phenylpyridine i-oxide measurements of the dependence of rate of nitration upon acidity in 75-81 % sulphuric acid at 25 °C show that both compounds are nitrated as their cations (table 8.1). The isomer distribution did not depend significantly upon the acidity, and by comparison with the kinetic data for quinolinium ( 10.4.2) the partial rate factors illustrated below were obtained.They should be compared with those for the nitration of 2-nitrobiphenyl ( 10.1). The protonated heterocyclic groups are much... 

In an intramolecular aldol condensation of a diketone many products are conceivable, since four different ends can be made. Five- and six-membered rings, however, wUl be formed preferentially. Kinetic or thermodynamic control or different acid-base catalysts may also induce selectivity. In the Lewis acid-catalyzed aldol condensation given below, the more substituted enol is formed preferentially (E.J. Corey, 1963 B, 1965B). 

Nevertheless, the puzzling fact to be explained is that the harder ring nitrogen prefers the softer electrophilic center and that this preference is more pronounced than the one observed for the amino nitrogen. Much remains to be done to explain ambident heterocyclic reactivity it was shown recently by comparison between Photoelectrons Spectroscopy and kinetic data that not only the frontier densities but also the relative symmetries of nucleophilic occupied orbitals and electrophilic unoccupied orbitals must be taken into consideration (308). 

Nucleophilic reactivity of the sulfur atom has received most attention. When neutral or very acidic medium is used, the nucleophilic reactivity occurs through the exocyclic sulfur atom. Kinetic studies (110) measure this nucleophilicity- towards methyl iodide for various 3-methyl-A-4-thiazoline-2-thiones. Rate constants are 200 times greater for these compounds than for the isomeric 2-(methylthio)thiazole. Thus 3-(2-pyridyl)-A-4-thiazoline-2-thione reacts at sulfur with methyl iodide (111). Methyl substitution on the ring doubles the rate constant. This high reactivity at sulfur means that, even when an amino (112, 113) or imino group (114) occupies the 5-position of the ring, alkylation takes place on sulfiu. For the same reason, 2-acetonyi derivatives are sometimes observed as by-products in the heterocyclization reaction of dithiocarba-mates with a-haloketones (115, 116). 

When unsubstituted, C-5 reacts with electrophilic reagents. Thus phosphorus pentachloride chlorinates the ring (36, 235). A hydroxy group in the 2-position activates the ring towards this reaction. 4-Methylthiazole does not react with bromine in chloroform (201, 236), whereas under the same conditions the 2-hydroxy analog reacts (55. 237-239. 557). Activation of C-5 works also for sulfonation (201. 236), nitration (201. 236. 237), Friede 1-Crafts reactions (201, 236, 237, 240-242), and acylation (243). However, iodination fails (201. 236). and the Gatterman or Reimer-Tieman reactions yield only small amounts of 4-methyl-5-carboxy-A-4-thiazoline-2-one. Recent kinetic investigations show that 2-thiazolones are nitrated via a free base mechanism. A 2-oxo substituent increases the rate of nitration at the 5-position by a factor of 9 log... 

The kinetics of the reaction between 2-methylthiothiazoles and methyl iodide show that the nucleophilic center is the ring nitrogen. The 2-methylthio group decreases the nucleophilicity of the this atom (269). 

Alkoxythiazoles are easily cleaved by acids yielding A-4-thiazoline-2-ones (36). C-5 Nitration of the thiazole ring is favored by the 2-alkoxy group (288. 297, 307). Recent kinetic investigations have shown that the rate enhancement is 3 log units (893). 

The mobility of the proton in position 2 of a quaternized molecule and the kinetics of exchange with deuterium has been studied extensively (18-20) it is increased in a basic medium (21-23). The rate of exchange is close to that obtained with the base itself, and the protonated form is supposed to be the active intermediate (236, 664). The remarkable lability of 2-H has been ascribed to a number of factors, including a possible stabilizing resonance effect with contributions of both carbene and ylid structure. This latter may result from the interaction of a d orbital at the sulfur atom with the cr orbital out of the ring at C-2 (21). 

On reaction with acyl chlorides and acid anhydrides phenols may undergo either acylation of the hydroxyl group (O acylation) or acylation of the ring (C acylation) The product of C acylation is more stable and predominates under conditions of thermodynamic control when alu mmum chloride is present (see entry 6 m Table 24 4 Section 24 8) O acylation is faster than C acylation and aryl esters are formed under conditions of kinetic control... 

Although the number of ring atoms is the structural feature upon which we focus attention, we shall use the criteria of thermodynamics and kinetics to assess the feasibility of the reactions listed above. 

On the basis of both thermodynamic and kinetic evidence-both of which are interpretable in terms of the strain associated with rings of certain sizes or similar structural factors we see that only rings with five or six atoms have any significant stability. Accordingly, we conclude the following ... 

Potassium Amides. The strong, extremely soluble, stable, and nonnucleophilic potassium amide base (42), potassium hexamethyldisilazane [40949-94-8] (KHMDS), KN [Si(CH2]2, pX = 28, has been developed and commercialized. KHMDS, ideal for regio/stereospecific deprotonation and enolization reactions for less acidic compounds, is available in both THF and toluene solutions. It has demonstrated benefits for reactions involving kinetic enolates (43), alkylation and acylation (44), Wittig reaction (45), epoxidation (46), Ireland-Claison rearrangement (47,48), isomerization (49,50), Darzen reaction (51), Dieckmann condensation (52), cyclization (53), chain and ring expansion (54,55), and elimination (56). 

Noncatalytic ring chlorination of toluene in a variety of solvents has been reported. Isomer distributions vary from approximately 60% ortho in hydroxyhc solvents, eg, acetic acid, to 60% para in solvents, eg, nitromethane, acetonittile, and ethylene dichloride (49,50). Reaction rates are relatively slow and these systems are particularly appropriate for kinetic studies. 

The reactions are highly exothermic. Under Uquid-phase conditions at about 200°C, the overall heat of reaction is —83.7 to —104.6 kJ/mol (—20 to —25 kcal/mol) ethylene oxide reacting (324). The opening of the oxide ring is considered to occur by an ionic mechanism with a nucleophilic attack on one of the epoxide carbon atoms (325). Both acidic and basic catalysts accelerate the reactions, as does elevated temperature. The reaction kinetics and product distribution have been studied by a number of workers (326,327). 

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