Epoxide polymers ring opening

The third and newest modified natural mbber available is epoxidized natural mbber (ENR). This modification was actually discovered as early as 1922 (50), although the elimination of ring opening and side reactions to give a purely epoxidized material took another 50 years or so to achieve (51). The resulting polymer is a new material, with properties totally different from natural mbber, as iadicated ia Table 5. 

Ester functions are not saponified under these ring opening conditions. However, a trans-a-acetoxy function hinders the epoxide opening reaction and a noticeable decrease in yield is observed in comparison to the cw-a-acetoxy isomer. The ring opening reaction is also dependent on the concentration of sulfuric acid. Polymer formation results when the acid concentration is too low and the reaction is markedly slower with excessive concentrations of acid. A 0.5% (vol./vol.) concentration of acid in DMSO is satisfactory. Ring opening does not occur when ethanol, acetone, or dioxane are used as solvent. 

An alternate way to make block copolymers involving PDMS blocks 124,125) is to have these chains fitted with epoxide functions at chain end, and to react them with a vinylic or dienic polymer carrying terminal COOH functions. Sequential addition of monomers has also been used, the ring opening polymerization of the cyclic trimer (D3) being initiated by the anionic site of a living polymer126). 

Porath, 1974). B/s-oxirane compounds also can be used to introduce epoxide groups into soluble dextran polymers in much the same manner (Boldicke et al., 1988 Bocher et al., 1992). The epoxide group reacts with nucleophiles in a ring-opening process to form a stable covalent linkage. The reaction can take place with primary amines, sulfhydryls, or hydroxyl groups to create secondary amine, thioether, or ether bonds, respectively (Chapter 2, Section 1.7). 

The simplest model compound is cyclohexene oxide III. Monomers IV, V and VII represent different aspects of the ester portion of I, while monomers VII and VIII reflect aspects of both the monomer I and the polymer which is formed by cationic ring-opening polymerization. Monomers IV-VII were prepared using a phase transfer catalyzed epoxidation based on the method of Venturello and D Aloisio (6) and employed previously in this laboratory (7). This method was not effective for the preparation of monomer VIII. In this specific case (equation 4), epoxidation using Oxone (potassium monoperoxysulfate) was employed. 

Oxidation is the first step for producing molecules with a very wide range of functional groups because oxygenated compounds are precursors to many other products. For example, alcohols may be converted to ethers, esters, alkenes, and, via nucleophilic substitution, to halogenated or amine products. Ketones and aldehydes may be used in condensation reactions to form new C-C double bonds, epoxides may be ring opened to form diols and polymers, and, finally, carboxylic acids are routinely converted to esters, amides, acid chlorides and acid anhydrides. Oxidation reactions are some of the largest scale industrial processes in synthetic chemistry, and the production of alcohols, ketones, aldehydes, epoxides and carboxylic acids is performed on a mammoth scale. For example, world production of ethylene oxide is estimated at 58 million tonnes, 2 million tonnes of adipic acid are made, mainly as a precursor in the synthesis of nylons, and 8 million tonnes of terephthalic acid are produced each year, mainly for the production of polyethylene terephthalate) [1]. 

Kim et al. [67] recently reported the synthesis of heterometallic chiral polymer (salen) Co-(Al, Ga, ln)Cl3 complexes 26-32 (Figure 10) and their use in the HKR of racemic epoxides. Polymeric salen catalysts showed very high reactivity and enantioselectivity at substantially lower catalyst loadings for the asymmetric ring opening of terminal epoxide to obtain the enantio-enriched products. The performance of catalysts is retained on multiple-use and do not suffer the problems of solubility and deactivation (Scheme 5). 

ARO reaction with phenols and alcohols as nucleophiles is a logical extension of HKR of epoxides to synthesize libraries of stereochemically defined ring-opened products in high optical purity. To this effect Annis and Jacobsen [69] used their polymer-supported Co(salen) complex 36 as catalyst for kinetic resolution of epoxides with phenols to give l-aiyloxy-2-alcohols in high yield, purity and ee (Scheme 17). Conducting the same reaction in the presence of tris(trifluoromethyl)methanol, a volatile, nonnucleophilic protic acid additive accelerates KR reaction with no compromise with enantioselectivity and yield. Presumably the additive helped in maintaining the Co(III) oxidation state of the catalyst. 

Boileau, S., Anionic Ring-Opening Polymerizations Epoxides and Episulfides, pp. 467 487 in Comprehensive Polymer Science, Vol. 3, G. C. Eastmond, A. Ledwith, S. Russo, and P. Sigwalt, eds., Pergamon Press, London, 1989. 

The stereochemistry of ring-opening polymerizations has been studied for epoxides, episul-fides, lactones, cycloalkenes (Sec. 8-6a), and other cyclic monomers [Pasquon et al., 1989 Tsuruta and Kawakami, 1989]. Epoxides have been studied more than any other type of monomer. A chiral cyclic monomer such as propylene oxide is capable of yielding stereoregular polymers. Polymerization of either of the two pure enantiomers yields the isotactic polymer when the reaction proceeds in a regioselective manner with bond cleavage at bond 1. 

In addition, the GMA/EDMA copolymer proved to serve as a basic unit for the fabrication of highly permeable bioreactors in capillary format. Trypsin immobilization after epoxide ring opening with diethylamine and attachment of glutaraldehyde is mentioned as the probably most prominent example [64], The immobilization of trypsin was also carried out using another class of reactive monolithic methacrylate polymer, which is based on 2-vinyl-4,4-dimethylazlactone, acrylamide, and ethylene dimethacrylate [65]. In contrast to GMA/EDMA, trypsin can directly be immobilized onto this kind of monolith, as the 2-vinyl-4,4-dimethylazlactone moieties smoothly react with weak nucleophils even at room temperature. 

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