Abstract
The E/Z stereocontrol in a C=C bond is a fundamental issue in olefin synthesis. Although the thermodynamically more stable E geometry is readily addressable by thermal Z to E geometric isomerization through equilibrium, it has remained difficult to undergo thermal geometric isomerization to the reverse E to Z direction in a selective manner, because it requires kinetic trapping of Z-isomer with injection of chemical energy. Here we report that a dinuclear PdI−PdI complex mediates selective isomerization of E-1,3-diene to its Z-isomer without photoirradiation, where kinetic trapping is achieved through rational sequences of dinuclear elementary steps. The chemical energy required for the E to Z isomerization can be injected from an organic conjugate reaction through sharing of common Pd species.
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Introduction
The E/Z stereocontrol of a C=C moiety has been a central issue in olefin chemistry. Significant efforts have been made to obtain the thermodynamically less stable Z-alkenes as a kinetically preferred product, because Z-alkenes are contained in many natural products, biologically active molecules, and synthons for organic synthesis1,2. Several bond-construction methods have been developed to obtain Z-alkene selectively, such as syn 1,2-adition to alkynes, stereoretentive cross-coupling using Z-vinyl reagents, Z-selective olefin metathesis, modified Wittig reactions, and Z-selective double bond migration3,4,5,6,7,8,9,10. In view of the fact that an E/Z mixture of alkenes in which a thermodynamically more stable E-alkene is the major isomer can be readily obtained by a common alkene construction method such as the Wittig reaction, the E to Z geometric isomerization may also become a powerful method to address to Z-alkenes. Despite its potential usefulness, however, the E to Z geometric isomerization of alkenes is not straightforward. Although photoirradiation of several alkenes leads to the E to Z isomerization1,11,12,13, Z stereoselection under photoirradiation is sometimes incomplete, mainly because a photochemical E/Z ratio depends on a photostationary state derived from an excited state structure1,14,15. Moreover, it has been difficult to undergo E to Z geometric isomerization without photoirradiation, because an equilibrium of a reversible E/Z isomerization lies largely to the side of E-alkenes (Fig. 1a). The claims that thermal E to Z isomerization of 1,3-dienes proceeds in the presence of a cobalt catalyst16 have proven erroneous recently. There has been no rational mechanism that allows kinetic trapping of Z-alkenes through a thermal E/Z isomerization. For example, E/Z geometric isomerization of alkenes is efficiently mediated or catalyzed by a transition metal hydride ([M]−H)17, where the production of Z-alkenes is disfavored due to the difficulty of kinetic discrimination of one of two diastereotopic β-H atoms during β-H elimination10, in addition to the rapid reversibility of migratory insertion and β-H elimination (Fig. 1b). Any other established mechanisms involving transition metal species such as (allylic C–H oxidative addition)-(reductive elimination), (allylic C–H radical abstraction)-addition, and (nucleophile/electrophile addition)-elimination18,19,20,21 also preferentially gives E-alkene over Z-alkene. It is noted that even a technique using 1,2-addition and 1,2-elimination reactions has been considered as a formal E to Z isomerization, in which an E-alkene is initially converted to an isolable C–C single bonded organic product through syn (or anti) addition, and then 1,2-anti (or syn) elimination reaction gives a corresponding Z-alkene22,23,24. Thus, it is highly desirable to develop a mechanism that enables straightforward, selective E to Z geometric isomerization of alkenes.
We envisioned that a dinuclear M–M bonded species might promote E to Z isomerization through a rational mechanism. Our strategy is based on the following hypotheses; i) an M–M bonded species that can accommodate alkenes at its semi-bridging or bridging coordination site undergoes stereoretentive syn addition to an E-alkene, ii) subsequent stereoinversion at the α-carbon center of the dimetalated intermediate generates the Z-equivalent intermediate, that then gives Z-alkene selectively via dinuclear syn elimination, and iii) as an alternative to ii), dinuclear anti elimination from the syn addition product gives Z-alkene selectively (Fig. 1c). Concerning the pathway i)→ii), the previous stereochemical study by our group proved that the dinuclear addition and elimination of a Pd–Pd moiety to/from 1,3,5-trienes occur in a highly stereoretentive (syn) manner, although the stereoinversion in a bi-π-allyl dinuclear adduct is very slow in the absence of Pd0 impurities25. If the stereoinversion at the α-carbon center occurs reversibly, the Z-equivalent intermediate is expected to become a major component because the metal moieties, which are usually the most sterically demanding groups, prefer an antiperiplanar conformation with a transoid R1–C–C–R2 geometry (Fig. 1c). The pathway i)→iii) may be considered when the stereoinversion at the α-carbon center is very slow or inaccessible, although the selective dinuclear anti elimination giving Z-alkenes has not been reported. When synthetically important 1,3-dienes are used as the alkene substrate, these mechanisms involve dimetallated intermediates having either η1-σ-M or η3-π-M (Fig. 1d)26,27.
Here, we report that a dinuclear PdI–PdI complex has the ability to mediate selective isomerization of E-1,3-diene to its Z-isomer without photoirradiation. We demonstrate that the sequence of dinuclear elementary steps involving either pathway i)→ii) or i)→iii) provides a rational way to obtain Z-1,3-dienes. Furthermore, we also show that the chemical energy required for the E to Z isomerization can be injected from an organic conjugate reaction through sharing of common Pd species, making the net process exergonic (Fig. 1a).
Results and discussion
A sequence of dinuclear addition, stereoinversion, and syn dinuclear elimination
We employed a dinuclear PdI–PdI bonded complex [Pd2(CH3CN)6][BF4]2 (1)28, which shows high reactivity with unsaturated hydrocarbons. We chose 1,3-dienes as the alkene substrate, not only because 1,3-dienes become useful starting substrates for many synthetic applications, but also because 1,3-dienes are smoothly introduced to the bridging coordination site of a dinuclear Pd–Pd27,29,30,31,32. We found that the reaction of 1 with either methyl E-5-methylhexa-2,4-dienoate (E-2) or its Z-isomer (Z-2) immediately gave an equilibrium mixture of transoid-antifacial and cisoid-antifacial isomers of the dinuclear adducts [Pd2(μ-η3:η1-mmd)(CH3CN)5][BF4]2 (3, mmd = methyl 5-methylhexa-2,4-dienoate) in a 92:8 molar ratio at 25 °C. The molar ratio of 3-transoid-antifacial:3-cisoid-antifacial reached 95:5 at −25 °C (Fig. 2a). The structures of these isomers were assigned by 1H-NMR and 13C-NMR analyses, where the vicinal coupling constant JH3–H4 of the transoid-antifacial isomer (JH3–H4 = 10.4 Hz) is larger than that of cisoid-antifacial one (JH3–H4 = 6.8 Hz), and the η1-bound 13C atom, which is located at the α-position with respect to the COOMe group, appeared at the high-field region (δ = 31 ppm for 3-transoid-antifacial). The molecular structure of the major isomer 3-transoid-antifacial was confirmed by X-ray structure analysis (Fig. 2b). The η3-bound Pd1 atom and the η1-bound Pd2 atom are antiperiplanar with each other, and the conformation around the C3–C4 bond is transoid. The C3–C4 bond length (1.446(12) Å) is longer than those of C1–C2 (1.413(11) Å) and C2–C3 (1.385(11) Å) due to its single bond character. The minor production of 3-cisoid-antifacial after the dinuclear addition to E-2 indicated that the stereoinversion of the dinuclear adduct 3 proceeded rapidly. That is, the syn dinuclear addition of 1 with E-2 initially gives 3-cisoid-antifacial, and subsequent stereoinversion occurs through the π–σ–π interconversion of the η3-allyl Pd moiety33,34, giving the thermodynamically more stable 3-transoid-antifacial in rapid equilibrium (Fig. 2c). As mentioned below, it was confirmed that the dinuclear addition of 1,3-diene to the Pd–Pd moiety proceeds in a stereoretentive (syn) manner when employing a 1,4-disubstituted 1,3-diene as the reactant. The theoretical calculations supported the relative stability of the dinuclear addition products; i.e., 3-transoid-antifacial is more stable by ΔG = 6.9 kJ/mol than 3-cisoid-antifacial; cf. Z-2 is in higher energy by ΔG = 8.3 kJ/mol compared to E-2.
We then examined the kinetic trapping of Z-2 from 3-transoid-antifacial through syn elimination (Fig. 2d), although the rapid π–σ–π allyl-Pd interconversion can cause elimination of E-2 via the reverse way of the formation of 3-transoid-antifacial from E-2. Bis(diphenylphoshino)methane (dppm) has been used as a good dinuclear eliminating reagent owing to its bridging coordination ability25,35, but addition of dppm to 3-transoid-antifacial showed poor Z-selectivity (E:Z = 80:20). Addition of PPh3 gave only E-2. P(OPh)3 showed improved but moderate Z-selectivity. Iodide also induced elimination of 2 with a moderate Z-selectivity (E:Z = 49:51), while 1,3-diene elimination with chloride or bromide was sluggish. We then examined the trans-olefination. Norton et al. previously revealed that the reversible trans-olefination of the diosmacyclobutane complex Os2(μ-η1:η1-C2H4)(CO)8 proceeds in a stereoretentive manner36,37. Our group also reported that the trans-olefination of the μ-η3:η3-1,3,5-triene Pd2 adduct with a linear 1,3,5-triene proceeds in a stereoretentive manner25. Although initial attempts of trans-olefination using 1,6-diphenyl-1,3,5-hexatriene gave only E-2, the use of 1,3,5-cycloheptatriene gave much better Z-selectivity (E:Z = 18:82). The trans-olefination with 1,3,5,7-cyclooctatetraene (COT) appeared to give a nearly perfect Z-selectivity (E:Z = 4:96) at −30 °C from the 95:5 mixture of the dimetallated intermediate 2. The 1H NMR analysis showed that [Pd2(μ-η3:η3-COT)(CH3CN)4][BF4]2 (4)38 was formed after the trans-olefination with COT. By using the present method, the Z-isomer of 2 and several other 1,3-dienes 5-8 having an ester group at one of the diene termini were obtained conveniently in 71–83% yields from the corresponding pure E-isomer (Fig. 2e). Typically, Z-2 was obtained by treatment of E-2 with 1 for 30 min at room temperature in CH3NO2 and subsequent addition of COT (2 equiv) at −30 °C for 15 min, where the Pd complex 4 can be easily removed by filtration after pouring the reaction mixture into Et2O, gave a crude product containing E-2:Z-2 = 9:91. It is noted that the observed high Z-selectivity is in contrast to the relatively lower selectivity of a previously reported photoinduced isomerization of 2; e.g., E-2:Z-2 = 40:60 from E-2 after irradiation with ultraviolet (UV)-light (254 nm)39. By using the present method, terminally aryl substituted dienes Z-9 and Z-10 were formed in low Z-selectivity (Fig. 2e) probably due in part to the concomitant formation of more than one dinuclear addition product; i.e., we observed unidentified isomers of the dinuclear adducts for these dienes by 1H NMR monitoring experiments.
A sequence of syn dinuclear addition and anti-dinuclear elimination
According to the mechanism shown in Fig. 2a, the E to Z isomerization of 1,4-disubstituted 1,3-dienes is not straightforward, because the corresponding dinuclear addition intermediate unlikely undergoes stereoinversion through π–σ–π allyl interconversion that accompanies the exchange of the syn/anti-substituents at the terminal η3-allyl moieties. In fact, it was confirmed that addition of 1 to the (2E,4E)- or the (2Z,4E)-isomer of methyl 5-phenylpenta-2,4-dienoate (11) in a CD3NO2-CD3CN solution (v/v = 9/1) proceeded in a highly stereospecific (syn) manner, yielding the transoid-antifacial or cisoid-antifacial dinuclear adduct [Pd2(μ-η3:η1-mpd)L5][BF4]2 (12-cisoid-antifacial or 12-transoid-antifacial, mpd = methyl 5-phenylpenta-2,4-dienoate) (Fig. 3a). The structure of each isomer of 12 was identified by the 1H NMR analysis, where the vicinal H3–H4 coupling constant of the transoid isomer (JH3–H4 = 10.4 Hz) is larger than that of the cisoid isomer (JH3–H4 = 6.0 Hz). We then examined the direct anti elimination from the E-equivalent intermediate 12-cisoid-antifacial that may give (2Z,4E)-11. For the anti elimination, we focused on the free-radical-induced metal elimination, since it is known that a metal–carbon bond undergoes homolysis by addition of radical species40,41,42. The double homolysis of the C–Pd bonds proceeded by addition of 2,2,6,6-tetramethylpiperidine 1-oxyl (TEMPO) (2 equiv) to 12-cisoid-antifacial in CD3NO2-CD3CN (v/v = 9/1) at −30 °C, giving (2Z,4E)-11 (76% yield, (2E,4E)-11:(2Z,4E)-11 = 24:76), where the mononuclear TEMPO-adduct [Pd(η2-TEMPO)(CH3CN)2][BF4] (13) was concomitantly formed (Fig. 3a). The TEMPO adduct 13 was isolated upon treatment of 1 with TEMPO in 91% yield, and its structure was determined by X-ray structure analysis (Fig. 3b). The observed Z-selectivity indicated that association of TEMPO to each PdII center in 12-cisoid-antifacial and subsequent Pd–C bond cleavage occurs with conservation of the cisoid geometry. The partial loss of the stereochemistry may be caused by the TEMPO-induced elimination mechanism, where a palladium moiety could eliminate in a stepwise manner. We confirmed that the treatment of 12-transoid-antifacial with TEMPO gave (2E,4E)-11 selectively (Fig. 3a). It is noted that treatment of 12-transoid-antifacial with COT resulted in the quantitative recovery of (2Z,4E)-11. For the preparative scale, in-situ-generated 12-cisoid-antifacial in CH3NO2–CH3CN (v/v = 95/5) from pure (2E,4E)-11 was treated with TEMPO (4 equiv) at −20 °C to give (2Z,4E)-11 in 56% yield (Fig. 3c). Other 1,4-disubstituted (2E,4E)-dienes such as 14, 15, and 16 were also isomerized to the corresponding (2Z,4E)-isomers in 27–64% yields (Fig. 3c). It was reported that UV-irradiation of (2E,4E)-11 at 313 nm gives a mixture of possible four isomers (2E,4E), (2Z,4E), (2E,4Z), and (2Z,4Z)-11 with low selectivity (18:16:34:32)39.
Injection of chemical energy through conjugate reactions
Finally, we demonstrated that the concept of conjugate reactions is applicable to the present E to Z isomerization of 1,3-diene, where the required chemical energy is injected from a coupled reaction by sharing of a common metal species (Fig. 1a). In biological systems, many endergonic chemical reactions are operated by energetic coupling with an exergonic reaction such as ATP-hydrolysis, that makes the net reaction system exergonic43. However, it is rare that the concept of the conjugate reaction system is applied to the reaction-design of artificial metal mediated-hill or catalyzed up-hill organic transformations. Although the above mentioned E to Z isomerization of 2 is driven thermodynamically by the organometallic complexation reaction of 1 with COT to yield the complex 4, a conjugate reaction system in which the E to Z isomerization is energetically coupled with a downhill reaction (A + B → C + D in Fig. 1a) could give a net exergonic system. Furthermore, regeneration of 1 after the coupled down-hill reaction is highly desirable. We developed the oxidative double amination of COT by using 1 for the organic coupled reaction. The reaction of 4 with a secondary amine such as pyrrolidine (2 equiv) at 0 °C in the presence of dibenzylideneacetone (dba) (5 equiv) gave a disubstituted 9-aza-barbaralane (17)44 (58% yield) and Pd2(dba)3 (18)45,46,47 (71% yield) (Fig. 4a). The molecular structure of the fluxional molecule 17 was confirmed by X-ray structure analysis (Fig. 4b). The formation of 17 might involve the nucleophilic amine-attack at one of the η3-allyl moieties in 4, subsequent deprotonation, intramolecular nucleophilic attack at the central carbon of the remaining η3-allyl moiety, and reductive elimination. The resultant Pd0 complex 18 can be converted to the PdI–PdI complex 1 in 90% yield by treatment with [Cp2Fe][BF4] in CH3CN–CH2Cl2 at room temperature (Fig. 4a), although the selective synthesis of a PdI2 complex by one-electron oxidation of Pd0 or one-electron reduction of PdII has been rarely reported48. Thus, merging the up-hill E to Z isomerization of 1,3-diene and the downhill oxidative double amination of COT gave a net exergonic conjugate reaction system, where delivery of the PdI–PdI species or its equivalent from one reaction to another gives a closed cycle (Fig. 4a).
For the anti elimination mechanism, the downhill oxidative protonation reaction of TEMPO becomes the coupled reaction for the up-hill E to Z alkene isomerization of 11. That is, protonation of the TEMPO-adduct 13 with HBF4·Et2O in CH3CN afforded [Pd(CH3CN)4][BF4]2 (19)49 in 80% yield with the elimination of [TEMPOH2][BF4] (20). The PdII complex 19 was then reduced with Cp2Fe in CH3CN to give 1 in 97% yield.
In summary, we have described E to Z isomerization of 1,3-dienes mediated by the dinuclear M–M bonded species. The E → Z stereocontrol can be achieved by a rational dinuclear mechanism that allows kinetic trapping of Z-1,3-diene. Furthermore, the concept of the conjugate reaction system demonstrated in this work may provide a basis to promote the metal-mediated up-hill organic transformation through energetic coupling with an exergonic reaction.
Methods
General procedure
All manipulations were conducted under a nitrogen atmosphere using standard Schlenk or drybox techniques. Unless specified, all reagents were purchased from commercial suppliers and used without purification. Solvents were purified according to the standard procedures. For experimental details, spectroscopic characterization data, X-ray crystallographic data, and details of quantum calculations, see the Supplementary Information.
Isomerization of methyl E-2 to Z-2
To a solution of [Pd2(CH3CN)6][BF4]2 (1, 126.5 mg, 2.00 × 10−1 mmol) in CH3NO2 was added methyl (E)-5-methylhexa-2,4-dienoate (E-2, 28.0 mg, 2.00 × 10−1 mmol) and stirred at room temperature for 30 min. The reaction mixture was cooled to −30 °C and COT (41.7 mg, 4.00 × 10−1 mmol, 2 equiv.) was added. After stirring 15 min, the mixture was diluted with diethyl ether, and filtered through a silica gel pad. The solvent was removed in vacuo and the residue was purified by a silica gel column chromatography to give methyl (Z)-5-methylhexa-2,4-dienoate (Z-2) as colorless oil (22.4 mg, 1.60 × 10−1 mmol, 80% yield, E:Z = <1:>99).
Isomerization of (2E,4E)-11 to (2Z,4E)-11
To a solution of [Pd2(CH3CN)6][BF4]2 (1, 168.1 mg, 2.66 × 10−1 mmol) in CH3NO2/CH3CN (v/v = 95:5) was added methyl (2E,4E)-5-phenylpenta-2,4-dienoate ((2E,4E)-11) (50.0 mg, 2.66 × 10−1 mmol) and stirred at room temperature for 15 min. The reaction mixture was cooled to −20 °C and a CH3NO2/CH3CN (v/v = 95:5) solution of TEMPO (167.7 mg, 1.07 mmol, and 4 equiv.) was added at −20 °C. After stirring 5 min, the mixture was diluted with diethyl ether, and filtered through Celite. The solution was washed with distilled water (two times). The organic layer was collected, and the aqueous layer was extracted with Et2O (two times). The combined organic layers were dried with MgSO4. The solvent was removed in vacuo and the residue was purified by a silica gel column chromatography and recycling size exclusion chromatography to give methyl (2Z,4E)-5-phenylpenta-2,4-dienoate ((2Z,4E)-11) as colorless oil (28.2 mg, 1.50 × 10−1 mmol, 56% yield, E:Z = <1:>99).
Synthesis of Pd2(dba)3 and 9-aza-barbaralane 17 through double amination of 4
To a solution of [Pd2(CH3CN)6][BF4]2 (1, 100.0 mg, 1.60 × 10−1 mmol) in CH3CN was added the COT (17.3 mg, 1.70 × 10−1 mmol) and stirred at room temperature. After 30 min, dba (185.1 mg, 7.90 × 10−1 mmol) was added to the reaction mixture, and then the reaction mixture was cooled at 0 °C. After addition of pyrrolidine (22.4 mg, 3.20 × 10−1 mmol) at 0 °C, the reaction mixture was stirred at the temperature for 2 h. The violet precipitate in suspension was then separated by decantation, and the supernatant was concentrated in vacuo. The solution was diluted with CHCl3, and filtered through a silica gel pad. The silica gel pad was washed with CHCl3. The product was extracted by MeOH/CHCl3 (v/v = 1:5), and concentrated in vacuo. The crude product was purified by a silica gel column chromatography (MeOH/CHCl3 (v/v = 1:10)) to give 9-aza-barbaralane 17 (24.2 mg, 9.00 × 10−2 mmol, 58% yield) as a red solid. The single crystal of 17 suitable for X-ray diffraction analysis was obtained by recrystallization from CH2Cl2/diethyl ether at −30 °C. The violet precipitate separated by decantation was washed with CH3CN and diethyl ether and dried in vacuo to yield Pd2(dba)3 (18) in 71% yield (Yield was determined by the free dba/Pd2(dba)3 molar ratio from 1H NMR).
Data availability
The authors declare that the data supporting the findings of this study are available within the paper and its supplementary information files, as well as from the corresponding author upon reasonable request. The X-ray crystallographic coordinates for structures reported in this study (3-transoid-antifacial, 13, and 17) have been deposited at the Cambridge Crystallographic Data Centre (CCDC), under deposition numbers 2003060-2003062. These data can be obtained free of charge from The Cambridge Crystallographic Data Centre via www.ccdc.cam.ac.uk/data_request/cif. The experimental data are available in Supplementary Information.
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Acknowledgements
H. Nakashima is acknowledged for his initial contribution to the 1,4-disubstituted 1,3-diene system. This work was supported by the grants-in-aid for scientific research from JSPS (JP18H04645, JP20H04805, JP17KT0102, JP18H01993, JP19H04565), and by JST-CREST (JPMJCR20B6).
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Chemical reaction experiments were performed by E.K., K.S., S.K., and K.Y. Theoretical calculations were performed by E.K. and K.Y. The manuscript was written by T.M. and K.Y. The present study was designed by T.M.
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Kudo, E., Sasaki, K., Kawamata, S. et al. Selective E to Z isomerization of 1,3-Dienes Enabled by A Dinuclear Mechanism. Nat Commun 12, 1473 (2021). https://doi.org/10.1038/s41467-021-21720-4
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DOI: https://doi.org/10.1038/s41467-021-21720-4
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