Activating groups substituents

Known leaving groups are X = I, Br, Cl, F, SPh, NMe3+, and OPO(OEt)2 (beware of the toxicity of this group). The reaction can be carried out without an activating group. Substituents OR, OPh, or COzH are tolerated,... 

Activating group Substituents speeding up a retiction, like electron-donating groups on benzene under electrophilic attack. 

The entrance of a third or fourth substituent can be predicted by Beilstein s rule. If a substituent Z- enters into a compound C H XY, both X and Y exert an influence, but the group with the predominant influence directs Z- to the position it will occupy. Since all meta-directing groups are deactivating, it follows that ortho—para activating groups predominate when one of them is present on the benzene ring. 

Fiber-Reactive Dyes. These dyes can enter iato chemical reaction with the fiber and form a covalent bond to become an iategral part of the fiber polymer. They therefore have exceptional wetfastness. Thein main use is on ceUulosic fibers where they are appHed neutral and then chemical reaction is initiated by the addition of alkaH. Reaction with the ceUulose can be by either nucleophilic substitution, using, for example, dyes containing activated halogen substituents, or by addition to the double bond in, for example, vinyl sulfone, —S02CH=CH2, groups. 

The effect of substituents on the reactivity of heterocyclic nuclei is broadly similar to that on benzene. Thus mem-directing groups such as methoxycarbonyl and nitro are deactivating. The effects of strongly activating groups such as amino and hydroxy are difficult to assess since simple amino compounds are unstable and hydroxy compounds exist in an alternative tautomeric form. Comparison of the rates of formylation and trifiuoroacetylation of the parent heterocycle and its 2-methyl derivative indicate the following order of sensitivity to substituent effects furan > tellurophene > selenophene = thiophene... 

Arenediazonium ions 1 can undergo a coupling reaction with electron-rich aromatic compounds 2 like aryl amines and phenols to yield azo compounds 3. The substitution reaction at the aromatic system 2 usually takes place para to the activating group probably for steric reasons. If the para position is already occupied by a substituent, the new substitution takes place ortho to the activating group. 

Decide whether p-ftrifluoromethvUbenzoic acid is stronger or weaker than benzoic acid. A substituent that strengthens the acid is a deactivating group because it withdraws electrons, and a substituent that weakens the acid is an activating group because it donates electrons. 

Probably the most widely applicable asymmetric imine aziridination reaction reported to date is that of Wulff et al. These workers approached the reaction from a different perspective, utilizing the so-called vaulted , axially chiral boron Lewis acids VANOL and VAPOL [35] to mediate reactions between ethyl diazoacetate and N-benzhydrylimines (Scheme 4.29) [36]. The reactions proceed with impressive enantiocontrol, but there is a requirement that the benzhydryl substituent be present since this group is not an aziridine activator there is, therefore, a need for deprotection and attachment of a suitable activating group. Nonetheless, this method is a powerful one, with great potential for synthesis, as shown by the rapid synthesis of chloroamphenicol by the methodology [37]. 

Compound la with no substitution, showed good activity with increased hpophihcity activity. Further increases in lipophihcity led to a decrease in activity. Replacement of a proton of the methyl group by a hpophobic group (chloro) resulted in a further decrease in activity. The order of activity of substituents at the first position was methyl, ethyl, unsubstituted, propyl, and chloromethyl. Compounds with a small substituent at Ci seem to provide optimum activity. As the test compounds could not be converted to water soluble form, in vitro evaluation for antihistaminic activity could not be performed. 

In a broad sense, one may include the Free-Wilson equation within the class of linear free energy relationships (LFER). It is also subjected to the assumption of additivity of the contributions to the biological activity by substituent groups at different substitution sites. The assumption requires, for example, that there is no hydrogen bonding interaction between the various substitution groups. 

More generally, many combinations of EWG substituents can serve as the anion-stabilizing and alkene-activating groups. Conjugate addition has the potential to form a bond a to one group and (3 to the other to form a a,y-disubstituted system. 

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