Chiral furanoside phosphite–phosphoroamidites: new ligands for asymmetric catalytic hydroformylation

We have designed a new series of phosphite–phosphoroamidites ligands 1–4 based on a furanoside backbone. These ligands were screened in the Rh-catalyzed asymmetric hydroformylation of styrene, inducing high regioselectivities with 2-phenylpropanal and moderate enantioselectivities (up to 65% e.e.). The results showed that the configuration of the stereogenic carbon atom C(3) at the ligand backbone had remarkable effects on the activity and enantioselectivity. Replacing the tert-butyl substituents with methoxy substituents at the para positions of the biphenyl moieties improved the enantioselectivities. We have also studied the solution structures of HRh(PP)(CO)₂ complexes.     

Application of a chiral scaffolding ligand in catalytic enantioselective hydroformylation

The synthesis of β-amino-aldehydes has been achieved through enantioselective hydroformylation of PMP-protected allylic amines. The reaction is accomplished by using a scalemic scaffolding ligand that covalently and reversibly binds to the substrate. These ligands behave like chiral auxiliaries because they are covalently attached to the substrate during hydroformylation; however, similar to traditional asymmetric ligands, they can be used in catalytic quantities. The directed hydroformylation of disubstituted olefins occurs under mild conditions (35 °C and 50 psi CO/H(2)), and Z-olefins afford excellent enantioselectivities (up to 93% ee).     

Shaping and enforcing coordination spheres: the implications of C3 and C1 chirality in the coordination chemistry of 1,1,1-tris(oxazolinyl)ethane ("trisox")

A key feature of tris(oxazolinyl)ethane ("trisox") ligands, which have shown broad scope in asymmetric catalysis, is the orientation and steric demand of their oxazoline substituents. This, along with the modularity of their synthesis determines their coordination chemistry. The possibility to combine oxazolines, in which the stereogenic centers adjacent to the N-donor atoms have different absolute configuration, whilst retaining their ability to coordinate as tripodal ligands, has been demonstrated by the synthesis of the enantiomerically pure C3-symmetric iPr-trisox(S,S,S) and C1-symmetric iPr-trisox(S,S,R) and their reaction with [Mo(CO)3(NCMe)3] yielding [Mo{iPr-trisox(S,S,S)}(CO)3] (1 a) and [Mo{iPr-trisox(S,S,R)}(CO)3] (1 b), respectively. The non-autocomplementarity of two homochiral trisox ligands at one metal center has been demonstrated by reaction of rac-C3 iPr-trisox with one equivalent of [Co(ClO4)2].6 H2O, giving the centrosymmetric heterochiral complex [Co(iPr-trisox)2](ClO4)2 (3), whereas an analogous reaction with the enantiopure ligand yielded a mixture of Co(II) complexes, which is characterized by the total absence of a [(trisox)2Co](+/2+) ion. The scope of the trisox ligand in terms of facial coordination to both early and late transition metals was demonstrated by the synthesis and structural characterization of the mononuclear complexes [ScCl3(iPr-trisox)] (4), [Fe(tBu-trisox)(NCMe)3](BF4)2 (5), and [Ru(eta6-p-cymene)(iPr-trisox)](PF6)2 (6). The facial coordination of their three ligating atoms to a metal center may be impeded if the transition-metal center stereoelectronically strongly favors a non-deltahedral coordination sphere, which is generally the case for the heavier d8-transition-metal atoms/ions. Reaction of iPr-trisox with [Rh(cod)2]BF4 led to the formation of the 16-electron d8-configured complex [Rh(iPr-trisox)(cod)](BF4) (7), which is oxidized by CsBr3 to give the Rh(III) complex [RhBr3(iPr-trisox)] (8) possessing a C3-symmetric structure with a kappa3-N-trisox ligand. The crystalline salts [M2(mu-Cl3)(iPr-trisox)2](PF6) (M=Fe(II): 9, Co(II): 10, Ni(II): 11), were prepared by addition of one molar equivalent of iPr-trisox and an excess of KPF6 to solutions of the anhydrous (FeCl2) or hydrated metal halides (CoCl2.6 H2O, NiCl2.6 H2O). All dinuclear complexes display weak magnetic coupling. For the mononuclear species [CuCl2(iPr-trisox)] (12) the removal of a chloride anion and thus the generation of a dinuclear chloro-bridged structure failed due to Jahn-Teller destabilization of a potential octahedral coordination sphere.     

Efficient Cluster-Based Catalysts for Asymmetric Hydrogenation of α-Unsaturated Carboxylic Acids

The new clusters [H(4) Ru(4) (CO)(10) (μ-1,2-P-P)], [H(4) Ru(4) (CO)(10) (1,1-P-P)] and [H(4) Ru(4) (CO)(11) (P-P)] (P-P=chiral diphosphine of the ferrocene-based Josiphos or Walphos ligand families) have been synthesised and characterised. The crystal and molecular structures of eleven clusters reveal that the coordination modes of the diphosphine in the [H(4) Ru(4) (CO)(10) (μ-1,2-P-P)] clusters are different for the Josiphos and the Walphos ligands. The Josiphos ligands bridge a metal-metal bond of the ruthenium tetrahedron in the "conventional" manner, that is, with both phosphine moieties coordinated in equatorial positions relative to a triangular face of the tetrahedron, whereas the phosphine moieties of the Walphos ligands coordinate in one axial and one equatorial position. The differences in the ligand size and the coordination mode between the two types of ligands appear to be reflected in a relative propensity for isomerisation; in solution, the [H(4) Ru(4) (CO)(10) (1,1-Walphos)] clusters isomerise to the corresponding [H(4) Ru(4) (CO)(10) (μ-1,2-Walphos)] clusters, whereas the Josiphos-containing clusters show no tendency to isomerisation in solution. The clusters have been tested as catalysts for asymmetric hydrogenation of four prochiral α-unsaturated carboxylic acids and the prochiral methyl ester (E)-methyl 2-methylbut-2-enoate. High conversion rates (>94?%) and selectivities of product formation were observed for almost all catalysts/catalyst precursors. The observed enantioselectivities were low or nonexistent for the Josiphos-containing clusters and catalyst (cluster) recovery was low, suggesting that cluster fragmentation takes place. On the other hand, excellent conversion rates (99-100?%), product selectivities (99-100?% in most cases) and good enantioselectivities, reaching 90?% enantiomeric excess (ee) in certain cases, were observed for the Walphos-containing clusters, and the clusters could be recovered in good yield after completed catalysis. Results from high-pressure NMR and IR studies, catalyst poisoning tests and comparison of catalytic properties of two [H(4) Ru(4) (CO)(10) (μ-1,2-P-P)] clusters (P-P=Walphos ligands) with the analogous mononuclear catalysts [Ru(P-P)(carboxylato)(2) ] suggest that these clusters may be the active catalytic species, or direct precursors of an active catalytic cluster species.     

Diphosphite ligands based on ribose backbone as suitable ligands in the hydrogenation and hydroformylation of prochiral olefins

Rh(I) and Ir(I) cationic complexes [M(cod)(PP)]BF₄ have been synthesised from diphosphite ligands 4–6 derived from ribofuranose. They have been used in the rhodium and iridium catalysed asymmetric hydrogenation of acrylic acid derivatives. Ribose derivative ligands 4–6 have also been used as auxiliaries in the Rh-catalysed hydroformylation of styrene. Hydroformylation results have been explained on the basis of the species formed under hydroformylation conditions. Comparative experiments with the related epimer d-(+)-xylose derivatives showed that the configuration of the product is controlled by the absolute configuration of the stereogenic carbon atom C-3.     

Chiral diphosphites derived from d-glucose in the copper-catalyzed conjugate addition of diethylzinc to cyclohexenone

A series of diphosphite ligands 1–3 derived from readily available d-(+)-glucose and bisphenol or binaphthol derivatives have been applied as ligands in the Cu-catalyzed 1,4-addition of diethylzinc to cyclohexenone. Excellent reaction rates (TOF>1200 h⁻¹) and good enantioselectivities (e.e. of up to 84%) were achieved. The modular nature of these ligands allows easy systematic variation in the configuration of the stereocenters (C(3), C(5)) at the ligand backbone and in the biaryl substituents, so the optimum configuration for maximum enantioselectivity in the asymmetric 1,4-addition can be determined. The results obtained show that the enantioselectivity induced by the ligand depends strongly on the absolute configuration of the C(3) stereogenic centre, while the sense of the enantiodiscrimination is predominantly controlled by the configuration of the biaryl groups of the phosphite moieties.     

Synthesis and application of a new bisphosphite ligand collection for asymmetric hydroformylation of allyl cyanide

A series of mono- and bidentate phosphites was prepared with (S)-5,5',6,6'-tetramethyl-3,3'-di-tert-butyl-1,1'-biphenyl-2,2'-dioxy [(S)-BIPHEN] as a chiral auxiliary and screened in the asymmetric hydroformylation of allyl cyanide. These hydroformylation results were compared with those of two existing chiral ligands, Chiraphite and BINAPHOS, whose utility in asymmetric hydroformylation has been previously demonstrated. Bisphosphite 11 with a 2,2'-biphenol bridge was found to be the best overall ligand for asymmetric hydroformylation of allyl cyanide with up to 80% ee and regioselectivities (branch-to-linear ratio, b/l) of 20 with turnover frequency of 625 [h(-)(1)] at 35 degrees C. BINAPHOS gave enantioselectivities up to 77% ee when the reaction was conducted in either acetone or neat but with poor regioselectivity (b/l 2.8) and activities 7 times lower than that of 11. The product of allyl cyanide hydroformylation using (R,R)-11 was subsequently transformed into (R)-2-methyl-4-aminobutanol, a useful chiral building block. Single-crystal X-ray structures of (S,S)-11 and its rhodium complex 19 were determined.     

Chiral diphosphites derived from D-glucose: new highly modular ligands for the asymmetric catalytic hydrogenation

A series of novel diphosphite ligands derived from readily available D-(+)-glucose have been synthesized. These ligands were screened in the Rh-catalyzed hydrogenation of a series of alpha,beta-unsaturated carboxylic acid derivatives. Both excellent enantioselectivities (ee up to >99%) and activities were achieved. The advantage of these ligands is that their modular nature allows an easy systematic variation in the configuration of the stereocenters (C-3, C-5) at the ligand backbone and in the biaryl substituents, so the optimum configuration for maximum enantioselectivity in asymmetric hydrogenation can be determined. Results show that enantiomeric excesses depend strongly on the absolute configuration of C-3 and slightly on the stereocenter carbon C-5, while the sense of the enantiodiscrimination is predominantly controlled by the configuration of the biaryls at the phosphite moieties. Moreover, the presence of bulky substituents at the ortho-positions of the biaryl diphosphite moieties has a positive effect on enantioselectivity.     

Highly enantioselective Rh-catalyzed hydrogenation based on phosphine-phosphite ligands derived from carbohydrates.

A new class of efficient catalysts was developed for the asymmetric hydrogenation of alpha,beta-unsaturated carboxylic acid derivatives by synthesizing a series of novel phosphine-phosphite ligands (4a-d) derived from readily available D-(+)-xylose. Excellent enantioselectivities (> 99%) were achieved under very mild reaction conditions (1 bar H(2) and 20 degrees C). Varying the biphenyl substituents in the phosphite moiety greatly affected the enantioselectivity in the hydrogenation reactions. The results also indicate that the sense of enantioselectivity is mainly controlled by the configuration of the phosphite moiety. (31)P[(1)H] NMR and kinetic studies on intermediates of the catalytic cycle show that the [Rh(P(1)-P(2))(enamide)]BF(4) species is the resting state and that the rate dependence is first order in rhodium and hydrogen pressure and zero order in enamide concentration.     

Design and synthesis of site directed maleimide bifunctional chelators for technetium and rhenium

A new family of heterobifunctional linkers (L1-L9) containing a terminus consisting of a tridentate donor set for coordination of the {M(CO)(3)}(+) core (M = Tc, Re), and a thiol reactive maleimide group has been prepared conveniently and in high yield under Mitsunobu reaction conditions by the coupling of an appropriate alcohol derivative with maleimide. The rhenium complexes [Re(CO)(3)(Lx)]Br (x= 1-9) were prepared in good yields from the reactions of the ligands and (NEt(4))(2)[Re(CO)(3)Br(3)] in refluxing methanol. The ligands and their Re complexes were characterized by (1)H and (13)C NMR, IR, and ESI-MS. Ligand L4 and [Re(CO)(3)(L5)]Br have been structurally characterized by X-ray crystallography. Photoexcitation of solutions of the complexes [Re(CO)(3)(Lx)]Br (x= 4-6) gives rise to intense and prolonged luminescence at room temperature (fluorescence lifetimes of ca. 16 micros). The ligands and their Re complexes react smoothly at the maleimide linker with sulfhydryl groups of peptides and proteins at room temperature in phosphate-buffered saline (PBS, pH 7.4) to form stable thioether bioconjugates. The photoluminescence properties of the labeled conjugates are similar to those of the parent complexes, but with even longer lifetimes. The ligands can also be labeled at room temperature with (99m)Tc to give chemically robust complexes. The corresponding hydrazinonicotinamide derivative N-[5-(6'-hydrazinopyridine-3'-carbonyl)aminopentyl]maleimide (L10) was also prepared. While coupling of L10 to cysteine ethylester and synthesis of the rhenium derivative [ReCl(3)(HYNIC-maleimide)(2)] were successfully accomplished, attempts to couple [ReCl(3)(HYNIC-maleimide)(2)] to glutathione or BSA yielded intractable mixtures.     

High-pressure investigations under CO/H2 of rhodium complexes containing hemispherical diphosphites

The two rhodium complexes [Rh(acac)(L(R))] (L(R)=(S,S)-5,11,17,23-tetra-tert-butyl-25,27-di(OR)-26,28-bis(1,1'-binaphthyl-2,2'-dioxyphosphanyloxy)calix[4]arene; 6: R=benzyl, 7: R=fluorenyl), each based on a hemispherical chelator forming a pocket about the metal centre upon chelation, are active in the hydroformylation of 1-octene and styrene. As expected for this family of diphosphanes, both complexes resulted in remarkably high selectivity towards the linear aldehyde in the hydroformylation of 1-octene (l/b≈15 for both complexes). Linear aldehyde selectivity was also observed when using styrene, but surprisingly only 6 displayed a marked preference for the linear product (l/b=12.4 (6) vs. 1.9 (7)). A detailed study of the structure of the complexes under CO or CO/H(2) in toluene was performed by high-pressure NMR (HP NMR) and FT-IR (HP-IR) spectroscopies. The spectroscopic data revealed that treatment of 6 with CO gave [Rh(acac)(CO)(η(1)-L(benzyl))] (8), in which the diphosphite behaves as a unidentate ligand. Subsequent addition of H(2) to the solution resulted in a well-defined chelate complex with the formula [RhH(CO)(2)(L(benzyl))] (9). Unlike 6, treatment of complex 7 with CO only led to ligand dissociation and concomitant formation of [Rh(acac)(CO)(2)], but upon addition of H(2) a chelate complex analogous to 9 was formed quantitatively. In both [RhH(CO)(2)(L(R))] complexes the diphosphite adopts the bis-equatorial coordination mode, a structural feature known to favour the formation of linear aldehydes. As revealed by variable-temperature NMR spectroscopy, these complexes show the typical fluxionality of trigonal bipyramidal [RhH(CO)(2)(diphosphane)] complexes. The lower linear selectivity of 7 versus 6 in the hydroformylation of styrene was assigned to steric effects, due to the pocket in which the catalysis takes place being less adapted to accommodate CO or larger olefins and, therefore, possibly leading to facile ligand decoordination. This interpretation was corroborated by an X-ray structure determination carried out for 7.     

Unsymmetric bidentate ligands in metal-catalyzed carbonylation of alkenes

Characteristic features of unsymmetric bidentate ligands, in which the two coordination atoms are not equivalent, are reviewed with a focus on their use in metal-catalyzed olefin carbonylations. High enantioselectivity for a variety of substrates was achieved using ligand 9 in Rh-catalyzed hydroformylation. Unsymmetric ligand 21e shows high productivity accompanied by high regio- and enantioselectivities in the Pd-catalyzed alternating copolymerization of 1-alkene with CO. The advantages of electronic unsymmetry are demonstrated especially in the spectroscopic observation of single steps involved in catalytic cycles.     

Furanoside diphosphines derived from d-(+)-xylose and d-(+)-glucose as ligands in rhodium-catalysed asymmetric hydroformylation reactions

Chirality transfer by furanoside diphosphines 1–3 was investigated in the Rh-catalysed asymmetric hydroformylation of prochiral olefins. In general, they induced high regioselectivities with branched aldehydes and moderate enantioselectivities of up to 58%. Improved activities were seen when a methyl substituent was introduced at C-(5) of the sugar residue. Systematic variation of the configuration at C-(5) suggests that there is a cooperative effect between stereocentres, which results in a matched combination for ligand 3 with (R)-configuration at the C-(5) stereogenic centre. Introduction of a methyl substituent at C-(5) induces a strong coordination preference. The solution structures of the species formed under hydroformylation conditions were also investigated.     

Efficient Cluster‐Based Catalysts for Asymmetric Hydrogenation of α‐Unsaturated Carboxylic Acids

The new clusters [H₄Ru₄(CO)₁₀(μ‐1,2‐P‐P)], [H₄Ru₄(CO)₁₀(1,1‐P‐P)] and [H₄Ru₄(CO)₁₁(P‐P)] (P‐P=chiral diphosphine of the ferrocene‐based Josiphos or Walphos ligand families) have been synthesised and characterised. The crystal and molecular structures of eleven clusters reveal that the coordination modes of the diphosphine in the [H₄Ru₄(CO)₁₀(μ‐1,2‐P‐P)] clusters are different for the Josiphos and the Walphos ligands. The Josiphos ligands bridge a metal–metal bond of the ruthenium tetrahedron in the “conventional” manner, that is, with both phosphine moieties coordinated in equatorial positions relative to a triangular face of the tetrahedron, whereas the phosphine moieties of the Walphos ligands coordinate in one axial and one equatorial position. The differences in the ligand size and the coordination mode between the two types of ligands appear to be reflected in a relative propensity for isomerisation; in solution, the [H₄Ru₄(CO)₁₀(1,1‐Walphos)] clusters isomerise to the corresponding [H₄Ru₄(CO)₁₀(μ‐1,2‐Walphos)] clusters, whereas the Josiphos‐containing clusters show no tendency to isomerisation in solution. The clusters have been tested as catalysts for asymmetric hydrogenation of four prochiral α‐unsaturated carboxylic acids and the prochiral methyl ester (E)‐methyl 2‐methylbut‐2‐enoate. High conversion rates (>94 %) and selectivities of product formation were observed for almost all catalysts/catalyst precursors. The observed enantioselectivities were low or nonexistent for the Josiphos‐containing clusters and catalyst (cluster) recovery was low, suggesting that cluster fragmentation takes place. On the other hand, excellent conversion rates (99–100 %), product selectivities (99–100 % in most cases) and good enantioselectivities, reaching 90 % enantiomeric excess (ee) in certain cases, were observed for the Walphos‐containing clusters, and the clusters could be recovered in good yield after completed catalysis. Results from high‐pressure NMR and IR studies, catalyst poisoning tests and comparison of catalytic properties of two [H₄Ru₄(CO)₁₀(μ‐1,2‐P‐P)] clusters (P‐P=Walphos ligands) with the analogous mononuclear catalysts [Ru(P‐P)(carboxylato)₂] suggest that these clusters may be the active catalytic species, or direct precursors of an active catalytic cluster species.     

Spiroketal‐Based Phosphorus Ligands for Highly Regioselective Hydroformylation of Terminal and Internal Olefins

A new class of bidentate phosphoramidite ligands, based on a spiroketal backbone, has been developed for the rhodium‐catalyzed hydroformylation reactions. A range of short‐ and long‐chain olefins, were found amenable to the protocol, affording high catalytic activity and excellent regioselectivity for the linear aldehydes. Under the optimized reaction conditions, a turnover number (TON) of up to 2.3×10⁴ and linear to branched ratio (l/b) of up to 174.4 were obtained in the Rh^I‐catalyzed hydroformylation of terminal olefins. Remarkably, the catalysts were also found to be efficient in the isomerization–hydroformylation of some internal olefins, to regioselectively afford the linear aldehydes with TON values of up to 2.0×10⁴ and l/b ratios in the range of 23.4–30.6. X‐ray crystallographic analysis revealed the cis coordination of the ligand in the precatalyst [Rh( 3 d )(acac)], whereas NMR and IR studies on the catalytically active hydride complex [HRh(CO)₂( 3 d )] suggested an eq–eq coordination of the ligand in the species.     

Betaine-induced assembly of neutral infinite columns and chains of linked silver(I) polyhedra with embedded acetylenediide

Ten polymeric silver(I) double salts containing embedded acetylenediide: [(Ag2C2)2(AgCF3CO2)9(L1)3] (1), [(Ag2C2)2(AgCF3CO2)10(L2)3]H2O (2), [(Ag2C2)(AgCF3CO2)4(L3)(H2O)]0.75 H2O (3), [(Ag2C2)(1.5)(AgCF3CO2)7(L4)2] (4), [(Ag2C2)(AgCF3CO2)7(L5)2(H2O)] (5), [(Ag2C2) (AgC2F5CO2)7(L1)3(H2O)] (6), [(Ag2C2)(AgCF3CO2)7(L1)3(H2O)]2 H2O (7), [(Ag2C2)(AgC2F5CO2)6(L3)2] (8), [(Ag2C2)2(AgC2F5CO2)12(L4)2(H2O)4]H2O (9), and [(Ag2C2)(AgCF3CO2)6(L3)2(H2O)]H2O (10) have been isolated by varying the types of betaines, the perfluorocarboxylate ligands employed, and the reaction conditions. Single-crystal X-ray analysis has shown that 1-4 all have a columnar structure composed of fused silver(I) double cages, with C2(2-) species embedded in its stem and an exterior coat comprising anionic and zwitterionic carboxylates. For 5 and 6, single silver(I) cages are linked into a beaded chain through both types of carboxylate ligands. In 7, two different coordination modes of L1 connect the silver(I) polyhedra into a chain. For 8, the mu(2)-O,O' coordination mode of L3 connects the silver(I) double cages into a chain. Compound 9 exhibits a two-dimensional architecture generated from the cross-linkage of double cages by C2F5CO2-, L4, and [Ag2(C2F5CO2)2] units. Similar to 9, 10 is also a two-dimensional structure, which is formed by connecting the chains of linked double cages through [Ag2(CF3CO2)2] bridging.     

Adsorption at the liquid-liquid interface in the biphasic rhodium catalyzed hydroformylation of olefins promoted by cyclodextrins: a molecular dynamics study

Using molecular dynamics (MD) simulations, we investigate the interfacial distribution of partners involved in the phase transfer rhodium catalyzed hydroformylation of olefins promoted by beta-cyclodextrins (beta-CDs). The beta-CDs, the reactant (alkene), product (aldehyde), several rhodium complexes (the catalyst, its precursor, and its alkene adduct) are simulated at the water-"oil" interface, where oil is represented by chloroform or hexane. It is shown that unsubstituted beta-CD and its 6-methylated and 2,6-dimethylated analogues adsorb at the interface, whereas the liposoluble permethylated CD does not. The precursor of the catalyst [RhH(CO)(TPPTS)3]9- (with triphenylphosphine trisulfonated TPPTS3- ligands) sits in water, but the less charged [RhH(CO)(TPPTS)2]6- catalyst and the [RhH(CO)(TPPTS)2(alkene)]6- reaction intermediate are clearly surface active. The TPPTS3- anions also concentrate at the interface, where they adopt an amphiphilic conformation, forming an electrical double layer with their Na+ counterions. Thus, the most important key partners involved in the hydroformylation reaction concentrate at the interface, thereby facilitating the reaction, a process which may be further facilitated upon complexation by CDs. These results point to the importance of adsorption at the liquid-liquid interface in the two-phase hydroformylation reaction of olefins promoted by beta-CDs and provide microscopic pictures of this peculiar region of the solution.     

Rhodium-catalyzed hydroformylation of 1-hexene in an ionic liquid: a molecular dynamics study of the hexene/[BMI][PF6] interface

We report a molecular dynamics study of biphasic systems involved in the rhodium-catalyzed hydroformylation of 1-hexene in the 1-butyl-3-methyl-imidazolium hexafluorophosphate ionic liquid ([BMI][PF(6)] IL). We first describe the neat [BMI][PF(6)] interfaces with hexene (the substrate) and heptanal (the linear reaction product) as organic phases. The former interface is molecularly sharp with BMI+ cations preferentially oriented "perpendicular" (i.e., pointing their butyl chains toward the organic phase), whereas hexene molecules tend to be somewhat parallel to the interface. The interface with heptanal is approximately twice as broad, due to BMI+...O(heptanal) attractions, and the solvent molecules are disordered at the interface. No IL ions solubilize in the organic phase(s) whereas ca. 2-3 hexene or heptanal molecules diffused into the IL phase. The presence of the CO and H2 gases does not modify the nature of the hexene/IL interface, as these gases are mainly solubilized in the organic phase, respectively, as diluted species and in the form of a "gaseous" droplet. In the IL phase, one finds a few CO monomers, whereas the less soluble H2 molecules spend only transient excursions. We next simulate the phase separation of "randomly mixed" IL/hexene liquids with the [RhH(CO)L(3)] precatalyst as a solute, comparing the PPh(3) to the TPPTS(3-) ligands (L). The phases separate much more slowly than in the case of classical liquids, and the neutral complex with PPh(3) ligands solubilizes in the hexene phase, displaying loose dynamical contacts with the IL interface. This contrasts with the -9 charged [RhH(CO)(TPPTS)(3)](9-) complex that sits "immobilized" on the IL side of the interface and is mainly solvated by BMI+ cations. Finally, we characterize the solvation of -6 charged [RhH(CO)(TPPTS)(2)](6-), [RhH(CO)(2)(TPPTS)(2)](6-), and [RhH(CO)(TPPTS)(2)(hexene)](6-) complexes involved as reaction intermediates in the hydroformylation reaction and of the free TPPTS(3-) ligand itself in the bulk IL.     

Bis-phosphites and bis-phosphinites based on distally-functionalised calix[4]arenes: coordination chemistry and use in rhodium-catalysed, low-pressure olefin hydroformylation

Six calix[4]arenes each bearing two non-cyclic PR2 units attached at distal phenolic oxygen atoms, p-Bu t-calix[4]arene-25,27-(OPR2)2-26,28-(OR')2(R = OPh; R'= Prn, L1; R = OPh; R'= CH2CO2Et, L2; R= OPh; R'= CO2 cholesteryl, L3; R = Ph; R'= Prn, 4; R = Ph; R'= CH2CO2Et, L5; R = Ph; R'= CO2cholesteryl, L6) have been synthesized and their coordinative properties investigated. The diphosphites L1-L3, where the P centres are separated by 12 bonds, readily form chelate complexes provided the complexation reaction is achieved either by using a starting complex that possesses good leaving groups or by operating under high dilution in order to avoid oligomer formation. Thus, the cationic complexes [Rh(COD)L1]BF4 and [Rh(COD)L3]BF4 were both formed in high yield by reacting the appropriate diphosphite with either [Rh(COD)(THF)2]BF4 or [Rh(COD)2]BF4. At high dilution, reaction of L3 with the neutral complex [PdCl2(COD)] afforded the chelate complex [PdCl2L3] in 90% yield. The reaction of one equiv. of L1 with [Rh(acac)(CO)2] resulted in the formation of [Rh(acac)L1] without requiring high dilution conditions. When the latter reaction was carried out with 0.5 equiv. of L1, the bimetallic complex [{Rh(acac)(CO)}2(eta]1-P,eta1-P'-L1)] was formed instead. Reaction at high dilution of with the cyclometallated complex [Pd(o-C6H4CH2NMe2)(THF)2]BF4 gave the expected chelate complex [Pd(o-C6H4CH2NMe2)]BF4. The latter slowly converts in solution to an oligomer in which the ligand behaves as a (eta1-P,eta1-P') bridging ligand, thus leading to a less strained structure. All six ligands, when mixed with [Rh(acac)CO2], effectively catalyse the hydroformylation of octene and styrene. In the hydroformylation of octene, the linear aldehyde selectivities observed with L2 and L3 are significantly higher (linear : branched =ca. 10) than those obtained with the other 4 ligands of this study and also with respect to PPh3. Molecular modelling shows that the lower rim substituents of and form tighter pockets about the metal centre than do the other ligands and so sterically favour the formation of Rh(n-alkyl) intermediates over that of Rh(i-alkyl) ones. In styrene hydroformylation, all ligands result in the formation of unusually high amounts of the linear aldehyde, the b : l ratios being all close to 65 : 35. The highest activities were found when using an L/Rh ratio of 1/1.     

Xantphite: A New Family of Ligands for Catalysis. Applications in the Hydroformylation of Alkenes

The novel bulky diphosphite (P∩P) ligands ( 3 and 4 ) based on the 2,7,9,9‐tetramethyl‐9H‐xanthene‐4,5‐diol ( 2 ) backbone were investigated in the Rh‐catalyzed hydroformylation of oct‐1‐ene, styrene, and (E)‐oct‐2‐ene. These diphosphites gave rise to very active and selective catalysts for the hydroformylation of oct‐1‐ene to nonanal with average rates>10000 (mol aldehyde)(mol Rh)⁻¹h⁻¹ (P(CO/H₂)=20 bar, T=80°, [Rh]=1 mM ) and maximum selectivities of 79% for the linear product. Relatively high selectivities towards the linear aldehyde (up to 70%, linear/branched up to 2.3) but very high activities (up to 39000 (mol aldehyde)(mol Rh)⁻¹h⁻¹) were observed for the hydroformylation of styrene in the presence of these bidentate ligands (P(CO/H₂)=2 – 10 bar, T=120°, [Rh]=0.2 mM ). Remarkable activities (up to 980 (mol aldehyde)(mol Rh)⁻¹h⁻¹) were achieved with these diphosphites for the hydroformylation of (E)‐oct‐2‐ene with selectivities for the linear product of 74% (l/b up to 2.8, P(CO/H₂)=2 bar, T=120°, [Rh]=1 mM ). A detailed study of the solution structure of the catalyst under catalytic conditions was performed by NMR and high‐pressure FT‐IR. The spectroscopic data revealed that under hydroformylation conditions, the bidentate ligands rapidly formed stable, well‐defined catalysts with the structure [RhH(CO)₂(P∩P)]. All the ligands showed a preference for an equatorial‐apical ( ea ) coordination mode in the trigonal bipyramidal Rh‐complexes, indicating that a bis‐equatorial ( ee ) coordination is not a prerequisite for highly selective catalysts.