E configurations

For these reasons, in the MCSCF method the number of CSFs is usually kept to a small to moderate number (e.g. a few to several thousand) chosen to describe essential correlations (i.e. configuration crossings, near degeneracies, proper dissociation, etc, all of which are often tenned non-dynamicaI correlations) and important dynamical correlations (those electron-pair correlations of angular, radial, left-right, etc nature that are important when low-lying virtual orbitals are present). 

It has to be emphasized that in this framework J is the angular momentum operatoi in ordinary coordinate space (i.e., configuration space) and 0 is a (differential) ordinary angular polar coordinate. 

If compounds have the same topology (constitution) but different topography (geometry), they are called stereoisomers. The configuration expresses the different positions of atoms around stereocenters, stereoaxes, and stereoplanes in 3D space, e.g., chiral structures (enantiomers, diastereomers, atropisomers, helicenes, etc.), or cisftrans (Z/E) configuration. If it is possible to interconvert stereoisomers by a rotation around a C-C single bond, they are called conformers. 

The configuration of pairs of isomeric 4-aryIidene-5-pyrazoIones, (Z)- and (E)-(117), was determined by H NMR data (72G491). When R is H, the E configuration is preferred when it is a methyl or a phenyl group, the Z configuration predominates. The presence of an exocyclic sulfur atom as in (118) lowers the interconversion barrier and the products... 

Evidence for that stereochemical course comes from the rearrangement of meso-3,4-dimethylhexa-1,5-diene 4, which yields the E.Z-configured diene 5 almost quantitatively. With a transition state of boatlike geometry, a Z,Z- or E,E-configured product would be formed." ... 

Apparently, the 1H NMR spectra of 1 //-azepines are invariant over substantial temperature ranges.61 However, temperature dependence has been noted69 in the 13CNMR spectra of some 1 -acyl-1 //-azepines, and is attributed to hindered rotation about the N-CO bond rather than to ring-inversion phenomena AG free enthalpies of activation for hindered rotation of 62-66 kJ moP1 have been calculated. E/Z-rotamcr ratios for l-aroyl-l//-azepines have been assessed and show a slight preference for the -rotamer 22 however, an X-ray structural analysis of l-(4-bromobenzoyl)-2-methyl-3.5,7-triphenyl-l//-azepine demonstrates that in the crystal state it is exclusively in the E configuration.22... 

When an enolate is forced to take the E configuration, e.g, the enolate derived from cyclohexanone, predominant formation of the anti-aldol might be expected. Surprisingly, early experiments gave more or less stereorandom results in that the reaction with benzaldehyde gave a ratio of. vvtt/ant/ -aldols of 48 521B 23, Contrarily, recent investigations24 reveal a substantial anti selectivity (16 84), which is lowered in a dramatic manner (50 50) by the presence of lithium salts. Thus, the low stereoselectivity in the early experiments may be attributed to impurities of lithium salts or lithium hydroxide. 

On the other hand, the predominant formation of the diastereomeric aldols 3 b results from the titanium enolate 1 b of (S )-5,5-dimethyl-4-tert-butyldimethylsilyloxy-3-hexanone. For this purpose, the ketone is first deprotonated with A-(bromomagnesio)-2,2,6,6-tetramethylpiperidine and the magnesium enolate, presumably (E) configurated, formed is thereby treated with hexamethylphosphoric triamide and triisopropyloxytitanium chloride. After sonification, the aldehyde is added to give predominantly aldol adducts 3b the diastereomeric ratio of 3b/2b surpasses 95 5 and the chemical yields range from 85 to 88%53b. 

Lithium and zinc tert-butyl phenylmethyl sulfoxide (1) and A-phenyl imines 2, in which the substituent R is alkenyl or aryl, react at —78 °C over 2 hours with high anti diastereoselection (d.r. >98.5 1.5)6. Shorter reaction times result in poorer yields, due to incomplete reaction. In contrast, the reaction of the sulfoxide anion with benzaldehyde is complete after 5 seconds, but shows poor diastereoselection. When the substituent R1 or R2 of the imine 2 is aliphatic, the substrates exhibit poor chemical reactivity and diastereoselection. The high anti diastereoselection suggests that if a chelated cyclic transition state is involved (E configuration of the imine), then the boat transition state 4 is favored over its chair counterpart 5. 

Scheme 5-14 may be called a two-dimensional system of reactions, in contrast to Scheme 5-1 which consists of a one-dimensional sequence of two acid-base equilibria. In Scheme 5-14 the (Z/E) configurational isomerism is added to the acid-base reactions as a second dimension . The real situation, however, is yet more complex, as the TV-nitrosoamines may be involved as constitutional isomers of the diazohydroxide. In order not to make Scheme 5-14 too complex the nitrosoamines are not included, but are shown instead in Scheme 5-15. The latter also includes the addition reactions of the (Z)- and ( )-diazoates (5.4 and 5.5) to the diazonium ion to form the (Z,Z)-, (Z,E)- and (2 2i)-diazoanhydrides (5.6, 5.7 and 5.8) as well as proto-de-nitrosation reactions (steps 10, 11 and 12). This pathway corresponds to the reverse reaction of diazotization, as amine and nitrosating reagent (nitrosyl ion) are formed in this reaction sequence.

If a monoarylacetylene (ArC = CH) is taken as a model for a transition state of an arenediazonium ion with a nucleophile Nu, two types of transition state can be visualized the first, 7.13, leads to the (Z)-azo compound 7.14, whereas the second, 7.15, results in the (E )-isomer 7.16 (Scheme 7-3). If the transition state is reactantlike (i.e., early on the reaction coordinate), repulsive interaction between the nucleophile and the aryl nucleus is small because the distance Nu-Np is still large. Therefore, the repulsion between the lone pair on Np and the aryl nucleus becomes the decisive factor. It favors an (E )-configuration of the Np lone pair with respect to the aryl nucleus (obviously it is energetically dominant compared with the repulsion between the lone pairs on Na and Np) therefore, transition state 7.13 is at a lower energy level, and Nu attacks NB in the (Z)-configuration. 

This crisscross or von Halban-White-type cyclization product is formed from the (E)-configured intermediate 87, which cannot undergo the 67r-electrocy-clization like the (Z)-configured isomer 88, to yield the benzannelation product 86 [78,79]. While the diastereoselectivity of the alkyne insertion must have been controlled by the electronic and not the steric factors of the substituents on the alkyne, the anti-configuration of the tricyclic system 85 was confirmed by an X-ray structure analysis [77]. 

Chemoselectivity plays an important role in the benzannulation reaction as five-membered rings such as indene or furan derivatives are potential side products. The branching point is again the rf-vinylcarbene complex D intermediate which maybe formed either as a (Z)- or an ( )-metallatriene the (E)-configuration is required for the cyclisation with the terminal double bond. (Z)-Metallatriene D, however, leads to the formation of furan derivatives H (Scheme 8). Studies on the formation of (E)- and (Z)-isomers discussing stereoelectronic effects have been undertaken by Wulff [17]. 

The splitting of the asymmetric peak is ascribed to a Jahn-Teller splitting of the excited state which latter involves the open e configuration e ... 

---