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Tautomerism of imidazole

The only example of ring-chain tautomerism of imidazoles is 1-hydroxy-4 -imidazoline-3-oxide (69MI86 78MI2, pp. 155,182). [Pg.255]

All triazoles, tetrazoles, and unsymmetrically substituted imidazoles and pyrazoles can exist in two tautomeric forms, e.g., 1 2 and 3 4. However, attempts to isolate the individual tautomers have been unsuccessful, always leading to one isomer (for summaries of this aspect of the tautomerism of imidazoles, see references 1 and 2). Although the isolation of both tautomers of a number of com-... [Pg.28]

In spite of the higher stability of imidazole-2-ylidenes and their metal complexes, tautomerization of imidazoles to the corresponding NHCs are also scarce processes. The relative stability of imidazole N- or C-metal bound isomers was computationally studied by Crabtree and Einsentein, who found a strong dependence on the nature of the metal fragment. Sundberg et al. published in 1974 the first example of N- to C-tautomerization of an imidazole ligand mediated by a Ru(II) complex (Scheme 29), but an acidic media was needed and very low yields were obtained. [Pg.92]

A multiply bonded nitrogen atom deactivates carbon atoms a or y to it toward electrophilic attack thus initial substitution in 1,2- and 1,3-dihetero compounds should be as shown in structures (110) and (111). Pyrazoles (110 Z = NH), isoxazoles (110 Z = 0), isothiazoles (110 Z = S), imidazoles (111 Z = NH, tautomerism can make the 4- and 5-positions equivalent) and thiazoles (111 Z = S) do indeed undergo electrophilic substitution as expected. Little is known of the electrophilic substitution reactions of oxazoles (111 Z = O) and compounds containing three or more heteroatoms in one ring. Deactivation of the 4-position in 1,3-dihetero compounds (111) is less effective because of considerable double bond fixation (cf. Sections 4.01.3.2.1 and 4.02.3.1.7), and if the 5-position of imidazoles or thiazoles is blocked, substitution can occur in the 4-position (112). [Pg.56]

Halogen atoms in the 2-position of imidazoles, thiazoles and oxazoles (542) undergo nucleophilic substitution reactions. The conditions required are more vigorous than those used, for example, for a- and y-halogenopyridines, but much less severe than those required for chlorobenzene. Thus in compounds of type (542 X = Cl, Br) the halogen atom can be replaced by the groups NHR, OR, SH and OH (in the last two instances, the products tautomerize see Sections 4.02.3.7 and 4.02.3.8.1). [Pg.104]

Annular tautomerism of azoles and benzazoles [the nonaromatic tautomers of imidazole 17, 2H and 4(5)H have been calculated at the MP2/6-31G level to be about 15 kcal mol less stable than the IH tautomer (95JOC2865)]. We present here the case of 4(5)-substituted imidazoles, different from the histamine, histidine, and derivatives already discussed. By analogy with these histamines, 4-methylimidazole 17a is often named distal [N(t)H] and 5-methylimidazole 17b, proximal [N(7t)H] (Scheme 9). [Pg.15]

JA4105) (Section V,A) (2) that of 1,2,3-triazole and 3(5)-methylpyr-azole and the reason why they are liquid at room temperature (89JCC426) (Section V,D,2) and (3) the tautomerism of C-methyl-pyrazoles and -imidazoles (90JA1303) (Section which have already all been dis-... [Pg.53]

A major part of the information available on positions of tautomeric equilibria 14a 14b of imidazoles stems from the basicity measurements... [Pg.177]

We do not discuss in detail the cases of tautomerism of heterocycles embedded in supramolecular structures, such as crown ethers, cryptands, and heterophanes, because such tautomerism is similar in most aspects to that displayed by the analogous monocyclic heterocycles. We concentrate here on modifications that can be induced by the macrocyclic cavity. Tire so-called proton-ionizable crown ethers have been discussed in several comprehensive reviews by Bradshaw et al. [90H665 96CSC(1)35 97ACR338, 97JIP221J. Tire compounds considered include tautomerizable compounds such as 4(5)-substituted imidazoles 1///4//-1,2,4-triazoles 3-hydroxy-pyridines and 4-pyridones. [Pg.38]

Free carbenes based on 1,2,4-triazole are not as numerous as those based on imidazole (70ZN(B)1421, 95AGE1021, 97JA6668, 98JA9100). The carbene complex 169 (Ar = Ph, p-Tol) is prepared by the [3 + 2] cycloaddition route from [W(CO)j(C+=NC-HCOOEt)]- and aryldiazonium (930M3241). Oxidative decomplexation causes tautomerization of the 1,2,4-triazole ligand, the products being 170 (Ar= Ph, i-Tol). [Pg.159]

Most electrophilic substitutions in benzimidazole (31 R = H) occur primarily in the 5-position. In multiple bromination the order followed, 5 > 7 > 6,4 > 2, parallels molecular orbital calculations. In benzimidazole itself the 4(7)- and 5(6)-positions are tautomerically equivalent. Fusion of a benzene ring deactivates C-2 to electrophilic attack to such an extent that it is around 5000 times less reactive than the 2-position of imidazole. Strong electron donors at C-5 direct halogenation to the 4-position, whereas electron-withdrawing groups favor C-4 or C-6 substitution (84MI21). [Pg.270]

Tanokura M (1983) 1 II-NMstudy R on the tautomerism of the imidazole ring of histidine residues I. Microscopic pK values and molar ratios of tautomers in histidine-containing peptides. Biochim Biophys Acta 742 576-585. [Pg.283]

A complicating factor in imidazoles is tautomerism. Imidazole tautomerizes rapidly in solution and consists of two identical tautomers. This becomes a problem, though, in an unsymmetrically substituted imidazole, and tautomerism means 4-methylimidazole is in equilibrium with 5-methylimidazole. Depending upon substituents, one tautomer may predominate. Tautomerism of this kind cannot occur with -substituted imidazoles it is totally dependent upon the presence of an N-H group. Tautomerism is also not possible with oxazoles or thiazoles. [Pg.433]

The tautomeric ratio of B to A for histidine in water (Eq. 2-6) has been estimated, using 15N- and 13C-NMR, as 5.0 when the a-amino group is proto-nated and as 2.5 when at high pH it is unprotonated.17 This tautomerism of the imidazole group is probably important to the function of many enzymes and other proteins for example, if Ne of structure A (Eq. 2-6) is embedded in a protein, a proton approaching from the outside can induce the tautomerism shown with the release of a proton in the interior of the protein, perhaps at the active site of an enzyme. The form protonated on Ns (B of Eq. 2-6), which is the minor form in solution, predominates in some positions within proteins.18... [Pg.46]

A detailed analysis of substituent effects on the pKa values of imidazoles and tetrazoles as well as benzimidazoles and naphthimidazoles has been made.308 The ortho effect is shown to parallel that of 2-substituted pyridines and quinolines47 190 and application of the Hammett equation to the tautomerism of these systems is also considered. The equation also satisfies the effect of substituents on the basicity of the nitrogen in the 1-position for 1-pyrazolines.309... [Pg.48]

See other pages where Tautomerism of imidazole is mentioned: [Pg.16]    [Pg.24]    [Pg.60]    [Pg.224]    [Pg.109]    [Pg.363]    [Pg.148]    [Pg.284]    [Pg.363]    [Pg.284]    [Pg.99]    [Pg.848]    [Pg.47]    [Pg.92]    [Pg.16]    [Pg.24]    [Pg.60]    [Pg.224]    [Pg.109]    [Pg.363]    [Pg.148]    [Pg.284]    [Pg.363]    [Pg.284]    [Pg.99]    [Pg.848]    [Pg.47]    [Pg.92]    [Pg.311]    [Pg.48]    [Pg.61]    [Pg.177]    [Pg.177]    [Pg.180]    [Pg.186]    [Pg.229]    [Pg.32]    [Pg.243]    [Pg.322]    [Pg.433]    [Pg.749]    [Pg.365]    [Pg.148]    [Pg.920]   
See also in sourсe #XX -- [ Pg.451 ]



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