Oligomeric groups

The addition of alcohols to form the 3-alkoxypropionates is readily carried out with strongly basic catalyst (25). If the alcohol groups are different, ester interchange gives a mixture of products. Anionic polymerization to oligomeric acrylate esters can be obtained with appropriate control of reaction conditions. The 3-aIkoxypropionates can be cleaved in the presence of acid catalysts to generate acrylates (26). Development of transition-metal catalysts for carbonylation of olefins provides routes to both 3-aIkoxypropionates and 3-acryl-oxypropionates (27,28). Hence these are potential intermediates to acrylates from ethylene and carbon monoxide. 

Perfluoropolyethers with the linear perfluoropropoxy repeat unit have been commercialized (28). They are prepared by the anionic oligomerization of tetrafluorooxetane followed by direct fluorination to remove the acyl fluoride end group as well as to fluorinate the remaining CH2 groups n can vary widely. 

Oligomerization and Polymerization Reactions. One special feature of isocyanates is their propensity to dimerize and trimerize. Aromatic isocyanates, especially, are known to undergo these reactions in the absence of a catalyst. The dimerization product bears a strong dependency on both the reactivity and stmcture of the starting isocyanate. For example, aryl isocyanates dimerize, in the presence of phosphoms-based catalysts, by a crosswise addition to the C=N bond of the NCO group to yield a symmetrical dimer (15). 

Commercially, polymeric MDI is trimerized duting the manufacture of rigid foam to provide improved thermal stabiUty and flammabiUty performance. Numerous catalysts are known to promote the reaction. Tertiary amines and alkaU salts of carboxyUc acids are among the most effective. The common step ia all catalyzed trimerizations is the activatioa of the C=N double boad of the isocyanate group. The example (18) highlights the alkoxide assisted formation of the cycHc dimer and the importance of the subsequent iatermediates. Similar oligomerization steps have beea described previously for other catalysts (61). 

Butene. Commercial production of 1-butene, as well as the manufacture of other linear a-olefins with even carbon atom numbers, is based on the ethylene oligomerization reaction. The reaction can be catalyzed by triethyl aluminum at 180—280°C and 15—30 MPa ( 150 300 atm) pressure (6) or by nickel-based catalysts at 80—120°C and 7—15 MPa pressure (7—9). Another commercially developed method includes ethylene dimerization with the Ziegler dimerization catalysts, (OR) —AIR, where R represents small alkyl groups (10). In addition, several processes are used to manufacture 1-butene from mixed butylene streams in refineries (11) (see BuTYLENEs). 

Other Higher Oleiins. Linear a-olefins, such as 1-hexene and 1-octene, are produced by catalytic oligomerization of ethylene with triethyl aluminum (6) or with nickel-based catalysts (7—9) (see Olefins, higher). Olefins with branched alkyl groups are usually produced by catalytic dehydration of corresponding alcohols. For example, 3-methyl-1-butene is produced from isoamyl alcohol using base-treated alumina (15). 

The orange-red titanium acetylacetone chelates are soluble in common solvents. These compounds are coordinately saturated (coordination number equals 6) and thus much more resistant to hydrolysis than the parent alkoxides (coordination number 4). The alkoxy groups are the moieties removed by hydrolysis. The initial product of hydrolysis is beheved to be the bis-hydroxy bis-acetylacetone titanate, (HO)2Ti(acac)2, which oligomerizes to a... 

These products are characterized in terms of moles of substitution (MS) rather than DS. MS is used because the reaction of an ethylene oxide or propylene oxide molecule with ceUulose leads to the formation of a new hydroxyl group with which another alkylene oxide molecule can react to form an oligomeric side chain. Therefore, theoreticaUy, there is no limit to the moles of substituent that can be added to each D-glucopyranosyl unit. MS denotes the average number of moles of alkylene oxide that has reacted per D-glucopyranosyl unit. Because starch is usuaUy derivatized to a considerably lesser degree than is ceUulose, formation of substituent poly(alkylene oxide) chains does not usuaUy occur when starch is hydroxyalkylated and DS = MS. 

The nature of the product strongly depends on the length of the hydroxy acid generally when the hydroxyl group is remote the yield of lactone drops significantly. For example, 10-hydroxydecanoic acid [1679-53-4] does not produce any decanoUde instead, the reaction proceeds by intermolecular oligomerization, and a complex mixture of di-, tri-, tetra-, and pentalactones results (90). However, when Pseudomonas sp. or Candida iylindracea]i 2Lses are incubated with 16-hydroxyhexadecanoic acid [506-13-8] hexadecanoUde is the predorninant product (91). 

Various techniques exist that make possible a normal mode analysis of all but the largest molecules. These techniques include methods that are based on perturbation methods, reduced basis representations, and the application of group theory for symmetrical oligomeric molecular assemblies. Approximate methods that can reduce the computational load by an order of magnitude also hold the promise of producing reasonable approximations to the methods using conventional force fields. 

An EB-curable struetural adhesive formulation usually eonsists of one or more crosslinkable oligomeric resins or prepolymers, along with such additives as reactive diluents, plasticizers, and wetting agents. The oligomer is an important component in terms of the development of mechanical properties. The adhesive and cohesive properties depend on the crosslink density, chemical group substitution, and molecular organization within the polymer matrix. Adhesion is achieved... 

The subunits of an oligomeric protein typically fold into apparently independent globular conformations and then interact with other subunits. The particular surfaces at which protein subunits interact are similar in nature to the interiors of the individual subunits. These interfaces are closely packed and involve both polar and hydrophobic interactions. Interacting surfaces must therefore possess complementary arrangements of polar and hydrophobic groups. 

Many enzymes (see Chapters 14 to 16) derive at least some of their catalytic power from oligomeric associations of monomer subunits. This can happen in several ways. The monomer may not constitute a complete enzyme active site. Formation of the oligomer may bring ail the necessary catalytic groups together to form an active enzyme. For example, the active sites of bacterial glutamine synthetase are formed from pairs of adjacent subunits. The dissociated monomers are inactive. 

Stable stannaethenes, >C=Sn<,d25 ) and stannaphosphenes, >Sn=P<,d3o have been reported and these, again, exploit the use of bulky groups to prevent oligomerization. 

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