Enantioselective hydrogenation BINAP complexes

BINAP complexes (7 in Fig. 7.7) are among the most efficient chiral catalysts for enantioselective hydrogenations, hydrosilylations, etc. Heterogeniza-tion of this complex is highly desired because of the high price of the complex. 

Iridium(III) hydride forms complexes with DIOP, BDPP (2,4-bis(diphenyl-phosphino)pentane), NORPHOS, and BINAP ligands to produce amines in 11 -80% ee.679 Similar modest results are obtained in the reduction of N-arylketimines with an iridium(HI) complex with (2S,3 S) -C HIRA PHOS as the chiral ligand.680 The indium complexes with chiral phosphinodihydrooxazoles catalyze the enantioselective hydrogenation of imines in supercritical carbon dioxide with up to 80% ee, but generally lower ee values are observed in... 

Limited progress has been achieved in the enantioselective hydrogenation of a,/ -unsaturated carboxylic acid esters, amides, lactones, and ketones (Scheme 26.10). The Ru-BINAP system is efficient for the hydrogenation of 2-methy-lene-y-butyrolactone, and 2-methylene-cyclopentanone [98]. With a dicationic (S)-di-t-Bu-MeOBIPHEP-Ru complex under a high hydrogen pressure, 3-ethoxy pyr-rolidinone could be hydrogenated in isopropanol to give (R)-4-ethoxy-y-lactam in 98% ee [39]. 

Enantioselective hydrogenation of / -keto phosphonates in the presence of an ( R)-BINAP-Ru complex under 1-4 atm H2 and at room temperature provides the (R)-yS-hydroxy phosphonates in up to 99% ee (Fig. 32.20) [69]. The sense of enantioface selection is the same as that observed in the reaction of / -keto carboxylic esters (see Fig. 32.14). A BDPP-Ru catalyst is also usable [70]. Similarly, / -keto thiophosphonates are hydrogenated with a MeO-BIPHEP-Ru catalyst with up to 94% optical yield [69 b]. 

Enantioselective hydrogenation of simple ketones catalyzed by BINAP/chiral diamine-Ru complexes is applied to the synthesis of biologically active compounds and a chiral phosphine ligand. Some examples are shown in Figure 32.44 [85 a, 87, 102, 128, 130, 135],... 

Takaya and co-workers46 found that BINAP-based Ru(II) dicarboxylate complexes 31 can serve as efficient catalyst precursors for enantioselective hydrogenation of geraniol (2E)-32 and nerol (2Z)-32. (R)- or (iS )-citroncllal 33 is obtained in nearly quantitative yield with 96-99% ee. The nonallylic double bonds in geraniol and nerol were intact. Neither double bond migration nor (fi)-/(Z)-isomerization occurred during the catalytic process. Furthermore, the S/C ratio was extremely high, and the catalyst could easily be recovered (Scheme 6-18). This process can be applied to the asymmetric synthesis of a key intermediate for vitamin E. 

Isomerization of allylic amines is another example of the application of the BINAP complex. Rh BINAP complex catalyzes the isomerization of N,N-diethylnerylamine 40 generated from myrcene 39 with 76-96% optical yield. Compound (R)-citronellal (R)-42. prepared through hydrolysis of (R)-41, is then cyclized by zinc bromide treatment.49 Catalytic hydrogenation then completes the synthesis of (—)-menthol. This enantioselective catalysis allows the annual production of about 1500 tons of menthol and other terpenic substances by Takasago International Corporation.50... 

From a practical point of view, the catalytic asymmetric hydrogenation of the corresponding diones will be the preferred method if high yields and high enantioselectivity can be ensured. Recently, over 98% yield with more than 99% ee has been achieved by optimizing the reaction conditions.64 For example, asymmetric hydrogenation of 2,4-pentanedione catalyzed by Ru-BINAP complex in the presence of hydrochloric acid gave 2,4-pentanediol in more than 95% yield and over 99% ee (Scheme 6-29).64... 

Scheme 6-30 shows that the halogen-containing complexes RuX2 (BINAP) are excellent catalysts With an S/C of over 103 or even 104, the enantioselective hydrogenation of methyl 3-oxobutanoate can still proceed well in methanol. The yield of the enantioselective reaction is almost 100%. 

It is well accepted that the asymmetric reduction of simple dialkyl ketones generally proceeds with low enantioselectivity.68 Ohkuma et al.69 reported that hydrogenation of simple ketones can be achieved using Ru(II) catalysts in the presence of diamine and alcoholic KOH in 2-propanol. Promising results have been achieved in the asymmetric hydrogenation of alkyl aryl ketones with a mixture of an Ru-BINAP complex, chiral diamine, and KOH (Scheme 6-33). 

Ru(II)-BINAP complexes (1) can effect enantioselective hydrogenation of pro-chiral ally lie and homoallylic alcohols, without hydrogenation of other double bonds in the same substrate.1 The alcohols geraniol (2) and nerol (3) can be reduced to either (R)- or (S)-citronellol (4) by choice of either (R)- or (S)-l. Thus the stereochemical outcome depends on the geometry of the double bond and the chirality... 

Asymmetric hydrogenation of prochiral ketones,s Ketones substituted in the a- or (3-position by diverse polar groups, particularly OH,OR,NR2,COOR, can undergo highly enantioselective hydrogenation catalyzed by BINAP-Ru complexes. A key factor of asymmetric induction is undoubtedly chelation of the carbonyl group and the hetero atom to the Ru atom. 

Asymmetric hydrogenation of fi-keto esters.7 The Ru(OAc)2(BINAP) complexes are ineffective catalysts for asymmetric hydrogenation of (i-keto esters, but on treatment with HX (2 equiv.) are converted into complexes with the empirical formula RuX2(BINAP), which are effective catalysts for this enantioselective hydrogenation. Complexes of (R)-BINAP catalyze hydrogenation to (R)-(S-hydroxy esters in >99% ee, whereas the enantiomeric (S)-P-hydroxy esters are obtained... 

The Ru2C14(BINAP)2[N(C2H5)3] complex (13, 36-37) is equally effective for this enantioselective hydrogenation. 

The procedure for the synthesis of the title compound is a representative example of asymmetric hydrogenation in the presence of BINAP-Ru(ll) diacetate.5 The method is based on the synthesis of BINAP-Ru(ll) dicarboxylate complexes and enantioselective hydrogenation of geraniol.7 The present method provides the first practical means for asymmetric synthesis of (S)- and (R)-citronellol. (S)-(-)-Citronellol of optical purity up to 92% can be obtained in a limited quantity from rose oil. A microbiological reduction of geraniol was reported to give enantiomerically pure (R)-(+)-citronellol. ... 

BINAP was introduced by Noyori [18], It has been particularly explored for reduction with ruthenium catalysts. While the first generation rhodium catalysts exhibited excellent performance with dehydroamino acids (or esters), the second generation of hydrogenation catalysts, those based on ruthenium /BINAP complexes, are also highly enantioselective for other prochiral alkenes. An impressive list of rather complex organic molecules has been hydrogenated with high e.e. s. 

The BINAP-Rh catalyzed hydrogenation of functionalized olefins has a mechanistic drawback as described in Section 1.2.1. This problem was solved by the exploitation of BINAP-Ru(ll) complexes.Ru(OCOCH3)2(binap) catalyzes highly enantioselective hydrogenation of a variety of olefinic substrates such as enamides, a, (3- and (3,y-unsaturated carboxylic acids, and allylic and homoallylic alcohols (Figure 1.9). " " Chiral citronellol is produced in 300 ton quantity in year by this reaction. ... 

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