Enantioselective electron transfer

Enantioselective electron transfer reactions are not possible in principle because the electron cannot possess chirality. Whenever the choice of enantiodifferentiation becomes apparent, it will occur in chemical steps subsequent (or prior) to electron transfer. Thus, enantioselectivities require a chiral environment in the reaction layer of electrochemical intermediates although asymmetric induction was report-... 

To our knowledge, topologically chiral molecules have not yet been resolved into enantiomers. However, we may anticipate that their energy barrier to racemization will be extremely high, compared to Euclidean chiral molecules. Therefore they are expected to be useful in enantioselective interactions or reactions. For example, it has been shown that tetrahedral copper(I) bis-2,9-diphenyl-l,10-phenanthroline complexes (which form the catenate subunits) are good reductants in the excited state [97] therefore the chiral Cu(I) catenates could be used for enantioselective electron-transfer reactions. Alternatively, the resolution of topologically chiral molecules would allow to answer fundamental questions, such as what are the chiroptical properties of molecular trefoil knots ... 

Trefoil knots, and therefore the molecular knots discussed in this section, are chiral (Figure 4-29). The resolution of a dicopper(I) knot prepared from a helical precursor containing the 1,3-phenylene-linked bis-phenanthroline ligand described above (LI 198) has been achieved by crystallisation of the racemic cation with (5)-(+)-l,l -binaphthyl-2,2 -diyl phosphate [343]. As commented by these authors, the preparation of optically pure knot complexes is of great potential interest in relation both to interactions with biological molecules and, where the complexed metal has more than one accessible oxidation state, to enantioselective electron transfer [344]. 

Scheme 10.12 gives some examples of enantioselective cyclopropanations. Entry 1 uses the W.s-/-butyloxazoline (BOX) catalyst. The catalytic cyclopropanation in Entry 2 achieves both stereo- and enantioselectivity. The electronic effect of the catalysts (see p. 926) directs the alkoxy-substituted ring trans to the ester substituent (87 13 ratio), and very high enantioselectivity was observed. Entry 3 also used the /-butyl -BOX catalyst. The product was used in an enantioselective synthesis of the alkaloid quebrachamine. Entry 4 is an example of enantioselective methylene transfer using the tartrate-derived dioxaborolane catalyst (see p. 920). Entry 5 used the Rh2[5(X)-MePY]4... 

Scheme 12.22. Concept for enantioselective meso epoxide opening by electron transfer.

Radical chemistry has seen tremendous progress in the past two decades and can now be considered as an eminent sub discipline in synthetic organic chemistry [1-6]. Diastereoselective radical chemistry is well established and many examples of enantioselective radical reactions have appeared in the recent literature. For reviews on diastereoselective radical chemistry see [7-11] for reviews on enantioselective radical chemistry see [12-16] and for reviews on conjugate additions, see [17,18]. This review will detail different ways to introduce asymmetry during a radical reaction. These transformations can be broadly classified into atom transfer reactions, reductive alkylations, fragmentations, addition and trapping experiments, and electron transfer reactions. 

Highly enantioselective 1,5-substitution reactions of enyne acetates are also possible under carefully controlled conditions (Eq. 4.31) [46]. For example, treatment of enantiomerically pure substrate 70 with the cyano-Gilman reagent tBu2CuLi-LiCN at —90 °C provided vinylallene 71 as a 1 3 mixture of E and 2 isomers with 20% and 74% ee, respectively. This mediocre selectivity might be attributable to race-mization of the allene by the cuprate or other reactive copper species formed in the reaction mixture. The use of phosphines as additives, however, can effectively prevent such racemizations (which probably occur by one-electron transfer steps) [47]. Indeed, vinylallene 71 was obtained with an ee of 92% for the E isomer and of 93% for the 2 isomer if the substitution was performed at —80 °C in the presence of 4 eq. of nBusP. Use of this method enabled various substituted vinylallenes (which are interesting substrates for subsequent Diels-Alder reactions Sect. 4.2.2) to be prepared with >90% ee. 

The enantioselective oxidative coupling of 2-naphthol itself was achieved by the aerobic oxidative reaction catalyzed by the photoactivated chiral ruthenium(II)-salen complex 73. 2 it reported that the (/ ,/ )-chloronitrosyl(salen)ruthenium complex [(/ ,/ )-(NO)Ru(II)salen complex] effectively catalyzed the aerobic oxidation of racemic secondary alcohols in a kinetic resolution manner under visible-light irradiation. The reaction mechanism is not fully understood although the electron transfer process should be involved. The solution of 2-naphthol was stirred in air under irradiation by a halogen lamp at 25°C for 24 h to afford BINOL 66 as the sole product. The screening of various chiral diamines and binaphthyl chirality revealed that the binaphthyl unit influences the enantioselection in this coupling reaction. The combination of (/f,f )-cyclohexanediamine and the (R)-binaphthyl unit was found to construct the most matched hgand to obtain the optically active BINOL 66 in 65% ee. 

One example of such a course is the Haverford Laboratory in Chemical Structure and Reactivity (146) that includes six projects, each of which involves sample preparation, sample analysis and some kind of determination of the properties of the substance prepared. The projects include organopalladium chemistry, porphyrin photochemistry, enantioselective synthesis, computer-aided modeling, enzyme kinetics and electron transfer reactions. 

Moderate enantioselectivity factors have also been found for electron transfer reactions between HRP or GO and resolved octahedral ruthenium or osmium complexes, respectively. In particular, the rate constants for the oxidation of GO(red) by electrochemically generated and enantiomers of [Os(4,4 - 2 ) ]3 + equal 1.68 x 106 and 2.34 x 106 M-1 s-1, respectively (25 °C, pH 7) (41). The spectral kinetic study of the HRP-catalyzed oxidation of and A isomers of the cyclo-ruthenated complex [Ru(phpy)(phen)2]PF6 (Pig. 21) by hydrogen peroxide has revealed similarities with the oxidation of planar chiral 2-methylferrocene carboxlic acid (211). In both cases the stereoseleci-vity factor is pH dependent and the highest factors are not observed at the highest rates. The kA/kA ratio for [Ru(phpy)(phen)2]PF6 is close to 1 at pH 5-6.5 but increases to 2.5 at pH around 8 (211). 

An enantioselective approach to cytotoxic nor-calamenenes via electron-transfer-driven benzylic umpolung of an arene tricarbonyl chromium complex. Synthesis 2003, 1851-1855. 

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