Metal–Ligand Cooperation Facilitates Bond Activation and Catalytic Hydrogenation with Zinc Pincer Complexes

A series of PNP zinc pincer complexes capable of bond activation via aromatization/dearomatization metal–ligand cooperation (MLC) were prepared and characterized. Reversible heterolytic N–H and H–H bond activation by MLC is shown, in which hemilability of the phosphorus linkers plays a key role. Utilizing this zinc pincer system, base-free catalytic hydrogenation of imines and ketones is demonstrated. A detailed mechanistic study supported by computation implicates the key role of MLC in facilitating effective catalysis. This approach offers a new strategy for (de)hydrogenation and other catalytic transformations mediated by zinc and other main group metals.


■ INTRODUCTION
In moving toward a more sustainable future, it is imperative to develop "green" chemical transformations that are both economical and free of waste generation. 1 The most successful metals employed in catalytic reactions have historically been the noble metals, which typically suffer from high price, low abundance, and toxicity. 2 Thus, in the past two decades, there has been a notable increase in efforts to develop both organocatalysts and catalysts based on main group metals, which are generally more abundant and cost-effective alternatives to the noble metals. 2−4 Furthermore, significant effort has focused on developing transformations that are atom-efficient or generate byproducts that are benign or useful in their own right (e.g., H 2 O and H 2 ). 5 With respect to utilizing molecular main group metal complexes for catalytic transformations, one common impediment is redox innocence, often nullifying their ability to undergo the fundamental organometallic reactions of oxidative addition and reductive elimination ( Figure 1). 3,6 For example, in homogeneous zinc, magnesium, and calcium catalyzed reactions, the metal is almost exclusively limited to the M 2+ oxidation state, and thus productive cycles depend on only sigma bond metathesis and/or insertion steps which do not alter the oxidation state of the metal. 2,4 Nonetheless, utilizing this paradigm, complexes of these metals and other main group metals have demonstrated versatile catalytic applications including hydroamination, 7 polymerization, 8 hydrosilylation, 9−12 hydroboration, 12 and hydrogenation 13−17 in which metal hydride intermediates are often speculated (and occasionally isolated). 18−20 Zinc, in particular, has shown activity for all of these transformations and is a promising metal due to its low cost, relatively high abundance, and low toxicity. 2,21,22  Our group is interested in leveraging metal−ligand cooperation (MLC), in which bond activation occurs across both metal and ligand, to effect transformations in an atomeconomical, waste-free fashion. 23 The MLC approach has long been demonstrated for advancements with the noble metals, and more recently with more abundant first row transition metals, for reversible bond activation resembling oxidative addition and reductive elimination ( Figure 1). 1,24−27 Importantly, the metal center does not change oxidation state in this process, and as a result, this activation mode could also be potentially operative with redox-innocent main group metals. 28 With respect to aromatization/dearomatization MLC with main group metals, Braunstein, Danopoulos and co-workers characterized a family of dearomatized lithium and potassium complexes, but bond activation with these complexes has not yet been demonstrated. 29 Most notably, Berben and coworkers have shown that aluminum complexes supported by a tridentate bis(imino)pyridine ligand can activate N−H and O−H bonds across the aluminum center and ligand. 30−32 Other examples with Group 13 metals have also been introduced and explored with similar application. 33 In the case of zinc, we are only aware of reports in which the ligand itself is implicated as a proton or electron reservoir, 34,35 and very recently, MLC was proposed to facilitate methanol activation en route to a characterized zinc methylcarbonate species in a novel CO 2 reduction process. 36 Nonetheless, direct observation of reversible H-X bond activation across any main group metal and ligand via aromatization/dearomatization is unknown, and main group metal−ligand cooperation remains an underexplored area.
Based on our previous efforts, we hypothesized that it should be possible to synthesize pincer complexes of main group metals, such as zinc, that could reversibly activate bonds by MLC in which the oxidation state of the metal remains unchanged. If so, zinc-ligand cooperation could be employed to catalyze useful transformations, such as (de)hydrogenation reactions, which typically occur at a transition metal center. Herein, we establish that both aromatized and dearomatized zinc complexes supported by the PNP ligand ( Figure 1) can be prepared and isolated in a straightforward manner. We demonstrate the ability of this system to heterolytically cleave and form H−H and N−H bonds. Finally, this new mode of bond activation by zinc is applied toward the additive-free, catalytic hydrogenation of imines and ketones.

■ RESULTS AND DISCUSSION
Access to a dearomatized zinc pincer complex is readily achieved via the reaction of the PNP tBu pro-ligand with dimethylzinc at 140°C in toluene to generate PNP tBu *ZnMe (1) concurrent with loss of methane (Scheme 1). This simultaneous deprotonation and complexation approach is analogous to the procedure employed to prepare lithium and potassium pincer complexes, 29 and is not uncommon in the synthesis of zinc alkyl and amido species. 8,37,38 In contrast to procedures employed in the preparation of traditional dearomatized transition-metal pincer complexes, 24 in this approach, the addition of base is obviated by the basic nature of dimethylzinc itself, which is capable of deprotonating the side arm of the ligand. Upon mixing, the colorless ligand and dimethylzinc starting materials form a bright yellow solution, which upon heating evolves gas and exhibits an orange/red color, atypical of Zn 2+ compounds but quite typical of dearomatized PNP pincer complexes. 29 From monitoring the reaction progress with 1 H and 31 P{ 1 H} NMR spectroscopy, we propose that the room temperature yellow intermediate is formed by coordination of the PNP tBu ligand to ZnMe 2 , and subsequent heating results in the loss of methane and formation of the orange/red complex 1 (see Supporting Information). The dearomatized compound, PNP tBu *ZnMe, exhibits several characteristic signals in solution by NMR spectroscopy. For example, in toluene-d 8 , multiplets at −0.02 ppm in the 1 H NMR spectrum and −3.47 ppm in the 13 C{ 1 H} NMR spectrum indicate the presence of a zinc methyl moiety coupled to two inequivalent phosphorus atoms. In addition, the inequivalent arms of the pincer ligand are distinguishable by both 1 H (doublet at 3.53 ppm and broad singlet at 2.62 ppm) and 13 C{ 1 H} (doublet at 57.43 ppm and doublet of doublets at 31.19 ppm) NMR spectra, associated with the deprotonated and protonated arms, respectively, as confirmed by HSQC and DEPTQ NMR experiments. Most evidently, the 31 P{ 1 H} NMR of 1 exhibits two distinct doublets (40.75 and 5.74 ppm), with J PP coupling constants of 18 Hz, indicative of the inequivalent phosphorus atoms, with similar shifts as the known lithium and potassium compounds. 29 Utilizing the same protocol, a dearomatized zinc ethyl compound, PNP tBu *ZnEt (2), was also prepared (Scheme 1). The zinc ethyl complex forms via a similar pathway, and its spectroscopic features essentially match that of 1 (see Supporting Information Table S2). Most diagnostically, the 31 P{ 1 H} NMR also exhibits two doublets (39.13 and 4.53 ppm; J PP = 15 Hz). The zinc amido complex, PNP tBu *ZnN-(SiMe 3 ) 2 (4), is also isolable, and is prepared via the reaction of PNP tBu ZnCl 2 (3) (see Supporting Information for preparation and characterization of 3) with 2 equiv of sodium bis(trimethylsilyl)amide (Scheme 1). As compared to 1 and 2, PNP tBu *ZnN(SiMe 3 ) 2 (4) also exhibits two resonances in the 31 P{ 1 H} NMR (35.20 ppm and −0.33 ppm), but unlike those of the corresponding methyl and ethyl derivatives, the peaks are singlets indicating no observable P−P coupling across the zinc center.
Single crystals of PNP tBu *ZnR (R = Me, Et) and PNP tBu *ZnN(SiMe 3 ) 2 were grown by cooling saturated pentane solutions to −32°C, and the molecular structures were determined by X-ray crystallography (Figure 2), confirming the formation of a monomeric, dearomatized zinc pincer complex in each case. The zinc center in 1 and 2 is pseudotetrahedral, distorting the PNP ligand quite substantially from its typically planar conformation. Supporting the  Table S1). Also in agreement with the spectroscopic data, the Zn−P distance of the ligand arm that remains protonated increases 1 < 2 ≪ 4 (2.675, 2.965, and 4.914 Å, respectively); in the case of 4, the second phosphorus arm is clearly unbound in the solid state, rendering the zinc center three-coordinate. As such, it is understandable that the 31 P{ 1 H} NMR spectrum of 1 and 2 exhibit two doublets (from P−P coupling), whereas that for 4 exhibits two singlets, indicating an open arm in solution.
Though a coordination number of four is common for zinc, three-coordinate zinc is less common but has been observed. 39 While the preparation of organozinc (RZnX) species is formally an oxidative addition of an organic RX to Zn 0 , these species are typically stoichiometric reagents; 40 thus, in moving toward catalytic applications, the development of molecular and recyclable zinc compounds that can perform bond activation is significant. We previously reported the activation of N−H bonds mediated by MLC with a dearomatized ruthenium complex. 41,42 We found that electron-deficient aniline derivatives reacted via aromatization/dearomatization MLC to afford ruthenium anilido complexes irreversibly. In the case of ammonia, aniline, and other amines, reversible addition was observed. Related palladium and copper chemistry has also been explored. 43 We began our reactivity studies with the room temperature addition of the electron-poor aniline derivative, H 2 NAr (Ar = 2-chloro-4-nitrophenyl), to 1, which resulted in the immediate formation of the aromatized complex, PNP tBu Zn(Me)NHAr (5), in which N−H activation has occurred across both the metal center and the ligand side arm (Scheme 1). 44 Notably, the oxidation state of the zinc center remains +2, in that the pincer ligand itself reassumes a neutral charge, with both the methyl and anilido moieties serving as X-type ligands. 45 In solution, NMR spectroscopy provides conclusive evidence of the formation of 5, indicating symmetrization of the pincer side arms. Specifically, the 31 P{ 1 H} NMR changes drastically from two doublets for 1 (vide supra) to a broad singlet at 24.76 ppm for 5 and the 1 H NMR displays a doublet for four hydrogen atoms at 2.99 ppm, demonstrating solution-state equivalence of the methylene side arms. NMR data suggest that the addition across the side arm is irreversible in the case of this weakly basic amine.
Single crystals of 5 suitable for X-ray diffraction were grown by slow diffusion of pentane into a toluene solution ( Figure 2). The molecular structure confirms activation of H 2 NAr across both the metal center and ligand. In the solid state, one of the phosphorus arms of the PNP tBu pincer ligand is detached from the metal center, rendering complex 5 tetrahedral. A tetrahedral geometry is quite common for four-coordinate zinc centers, 46 and the conformation also resembles the structure found for PNP tBu ZnCl 2 (see Supporting Information); however, the NMR spectroscopy data indicate an equivalence of the side arms in solution consistent with a fivecoordinate zinc center, hinting that there may be a difference between the solid and solution state behavior for both 3 and 5. To probe this difference, a variable temperature NMR experiment was performed for 5. At low temperature, inequivalence of the methylene and tert-butyl groups on the side arms by 1 H NMR ( Figure 3) and the phosphorus linkers by 31 P{ 1 H} NMR (see Supporting Information) could be observed. Decoalescence of the signals is observed around 253 and 238 K in the 1 H NMR and 31 P{ 1 H} NMR spectra, respectively. We also performed the analogous experiment with compound 3 and observed the same phenomenon (see Supporting Information). These experiments confirm the labile nature of the phosphorus linkers in solution and are  (14), (2). See Supporting Information for molecular structure of 3. Journal of the American Chemical Society pubs.acs.org/JACS Article significant in that the hemilability of the side arm of PNP tBu complexes has been proposed, but, to our knowledge, has never been demonstrated experimentally. This finding is meaningful in that hemilability in pincer complexes has been extensively studied 47−51 and is believed to be significant in catalytic mechanisms of related compounds. 52 Most interestingly, addition of the more basic N-benzylaniline (PhN(H)Bn) to 1 under ambient conditions resulted in an observable equilibrium. Analysis of a mixture of PNP tBu *ZnMe (1) and PhN(H)Bn by 1 H and 31 P{ 1 H} NMR spectroscopies indicates the formation of an equilibrium mixture containing three major species: free amine, the dearomatized zinc methyl complex with coordinated amine (6), 53  Compound 7 is characterized as a component of the equilibrium mixture by NMR spectroscopy. Specifically, diagnostic signals at 23.19 ppm in the 31 P{ 1 H} NMR spectrum for the solution-state equivalent phosphorus atoms and at 4.33 ppm in the 1 H NMR spectrum for the −CH 2 Ph moiety in the amido ligand are observed. In addition, a small amount (<5%) of a species tentatively identified as PNP tBu *ZnNPhBn is formed. This species exhibits 31 P{ 1 H} NMR characteristic signals similar to 1 and is presumably formed from protolytic cleavage of the Zn−Me bond. The equilibrium between complexes 1, 6, and free amine and complex 7 could be probed by NMR spectroscopy via a variable temperature NMR study. Specifically, a d 8 -toluene solution of a roughly equimolar mixture of PNP tBu *ZnMe and N-benzylaniline was heated in increments from room temperature to 120°C, allowing the overall equilibrium between 1 and 7 to be established at each temperature. K eq was determined by integration of the corresponding 1 H NMR spectra, and a Van't Hoff plot permitted extraction of thermodynamic quantities (see Supporting Information). K eq over the temperature range was found to be between 1 and 100, with an experimentally determined K eq of 68.8 for the equilibrium mixture at 298 K, associated with a ΔG of −2.4 kcal/mol, which agrees reasonably well with our computed results (+1.1 kcal/mol at 393.15 K and 1 M standard states, vide infra). Observation of this equilibrium provides evidence that (i) free amine can coordinate to and then react with 1 via MLC to rearomatize the ligand and generate 7, (ii) free amine can be released by MLC to regenerate 1, and (iii) the reactants and product are quite similar energetically, such that the equilibrium is observable in solution by NMR spectroscopy. This unprecedented reversible N−H bond activation by MLC with a main group metal resembles transition-metal-like behavior.
Subsequently, we turned our attention to the activation of a nonpolar, environmentally relevant substrate, H 2 . Oxidative addition of H 2 to a transition metal is very important in several transition-metal catalyzed processes, 54 and we have observed reversible H 2 activation by MLC with related transition metal systems with applications in (de)hydrogenation catalysis. 24,55 Thus, we explored whether PNP tBu *ZnMe could potentially activate hydrogen, a challenging nonpolar bond, in the same fashion as the N−H bond. Treatment of a solution of 1 in toluene with 5 bar of H 2 in a high-pressure J. Young tube resulted in no significant change, even upon gradual heating to 80°C. Heating the sample at 90°C, however, resulted in partial decomposition, with gray precipitation presumed to be Zn 0 and the formation of the pro-ligand, PNP tBu . The reaction could be driven to completion by heating at 120°C for 2 days. We hypothesized that if H 2 activation was indeed occurring via MLC, a zinc hydride species, PNP tBu Zn(Me)H (8H, Scheme 2), may be an intermediate in this decomposition pathway. Note that numerous zinc hydride complexes have been described in the literature. 2,18 Additionally, computation indicates that 8H is only 2.5 kcal/mol higher in energy than 1 and free hydrogen, but that a barrier of 33.3 kcal/mol exists to split the H 2 molecule by MLC (vide inf ra). This suggests that while 8H may be accessible, it might be unstable under the conditions required for its generation. As such, we performed the hydrogen addition again at 120°C in a toluene solution, but now in the presence of a free imine, Nbenzylideneaniline, in order to possibly trap the in situ formed hydride. Gratifyingly, we observed no decomposition, and instead, formation of the aforementioned equilibrium mixture of complexes 1, 6, and free amine and complex 7 (Scheme 2) by 1 H and 31 P{ 1 H} NMR spectroscopy. This result likely implicates insertion of the imine into a Zn−H bond and also hinted at possible catalytic hydrogenation applications.
To further our understanding of the proposed H 2 activation via MLC, a solution of complex 1 in toluene was treated with 5 bar of D 2 . After heating at 90°C for 36 h, in addition to the observation of some decomposition, 2 H NMR spectroscopy confirmed that deuterium was incorporated into both side arms of 1 (14% incorporation). After further heating at 120°C for 1 week, similar to our observations with H 2 , complete decomposition of 1 occurred to a major species (>95%) with spectroscopic properties similar to the reprotonated PNP tBu ligand; the 2 H NMR spectrum and integration of the methylene protons in the 1 H NMR spectrum confirmed incorporation of deuterium (45% incorporation) into the free ligand arms (Scheme 2). In addition, a gray solid, again presumed to be Zn 0 , was observed lining the walls of the NMR tube, and both CH 3 D and CH 4 were detected by 1 H NMR spectroscopy (see Supporting Information). 56 This result further suggests the activation of H 2 (and D 2 ) via MLC. Moreover, observable incorporation of deuterium into 1 and the 45% deuterium incorporation into the free ligand at the end of the reaction both imply that the H 2 /D 2 activation is reversible. While dihydrogen has been utilized as the hydride source in the preparation of zinc hydride derivatives, 13,57 we Nonetheless, it is noteworthy that the relatively low incorporation likely indicates that the decomposition pathway in the absence of imine is facile as compared to the reverse dehydrogenation process. Finally, to confirm the role of the zinc center in the H 2 /D 2 activation, a control experiment was performed with the PNP tBu free ligand and D 2 . No incorporation of deuterium into the side arms was observed when employing the same conditions (see Supporting Information). Based on the unique activity of the main group metal zincbased pincer complex toward H 2 cleavage, insertion, and reversible activation of N−H bonds (vide supra), we posited that leveraging MLC might permit hydrogenation of polar unsaturated bonds with this system. To our knowledge, zinc catalyzed hydrogenation has been demonstrated for imines under very high H 2 pressures (68−100 bar) 13,14 and ketones with limited scope and high H 2 pressure (100 bar). 58 Reductions catalyzed by molecular zinc compounds utilizing other hydrogen sources, specifically hydrosilanes and hydroboranes, have been demonstrated, including imines, ketones, aldehydes, and nitriles. 2,10,11,59 The lack of reports of hydrogenation, we believe, is related to the energetic cost of sigma bond metathesis to split hydrogen and release product (hence the success of other hydrogen sources with more favorable thermodynamic driving forces). Given the ability of the aromatization/dearomatization MLC approach to facilitate the reversible activation of H 2 and N−H bonds in this pincer system, we hypothesized that these alternate pathways could potentially bypass other more energetically demanding routes with less favorable thermodynamics, thus allowing hydrogenation at milder conditions compared to previously reported studies.
Indeed, PNP tBu *ZnMe (1) is a moderately active catalyst for the hydrogenation of a model substrate, N-benzylideneaniline (Table 1, entry 1), at substantially lower pressures (7 bar) than the previous reports (68−80 bar) of zinc-catalyzed imine hydrogenation. 13,14 Specifically, when 0.5 mmol of Nbenzylideneaniline in 1.8 mL toluene was treated with 7 bar of H 2 in the presence of 1 (2.5 mol %) at 120°C, the corresponding amine was observed by GC-MS and 1 H NMR spectroscopy in up to 89% yield after 18 h. Various substituted benzylideneaniline derivatives, with both electron-donating and electron-withdrawing groups on the phenyl ring, were also hydrogenated to their corresponding amines under similar conditions with high to excellent yields (entries 2−6). Upon changing the R″ group on nitrogen from phenyl to alkyl moieties, higher pressure was needed to obtain substantial conversion (entries 7−10). Interestingly, N-benzylidene-tertbutylamine was not amenable to hydrogenation under the reaction conditions, most probably due to the bulky t Bu group (entry 8). On the other hand, as the R″ group was changed to a less bulky alkyl group (Me, Bn), hydrogenation to the corresponding amine products was observed (entries 7 and 9). R′ on carbon is not limited to aromatic substituents; while aldimines with aliphatic R′ are relatively elusive, we also found that N-butylbenzylamine can be prepared from the corresponding imine, N-butylidenebenzylamine, in moderate yield with a somewhat longer reaction time (entry 10). Finally with respect to imines, we demonstrate that 1 also catalyzes hydrogenation of a ketimine, specifically phenyl-(1-phenylethylidene)amine, in good yield (entry 11).
While several main group metals exhibit activity for imine hydrogenation, homogeneous ketone hydrogenation by main group metals is exceptionally limited. The reported examples involve extremely high pressures, 58,60,61 the use of additives, 62 or a narrow substrate scope. 58,60,63 Thus, it is significant that we found that 1 can catalyze the hydrogenation of ketones with aromatic, aliphatic, and mixed aromatic/aliphatic R and R′ Journal of the American Chemical Society pubs.acs.org/JACS Article substituents under 65 bar of H 2 at 140°C. Specifically, benzophenone is hydrogenated to diphenylmethanol in up to 88% yield (entry 12). Additionally, compound 1 catalyzes hydrogenation of 4-heptanone to 4-heptanol and propiophenone to 1-phenyl-1-propanol in good yield (entries 13−14). With respect to green chemistry, utilizing zinc is inherently significant for these transformations, but also, it is important that (i) there is no need for any base or other additives and (ii) the process is 100% atom economical (as opposed to previously reported zinc reductions with hydrosilanes and hydroboranes). 59,64 Mechanistically, we propose a plausible cycle (Figure 4) accounting for the observations from the stoichiometric and catalytic experiments. In the first step, the arm of PNP tBu *ZnMe (A) can open (B) allowing for the reversible activation of hydrogen by MLC to generate an aromatized zinc hydride intermediate (C). In the presence of imine or ketone, rather than decomposing, the zinc hydride can be trapped via an insertion pathway, generating the aromatized zinc amido or alkoxy complex (E) (vide supra, Scheme 2). Several pathways seem plausible for the insertion to proceed, but here we propose one concerted path (direct to E) and one stepwise path (via D; see Supporting Information). Insertion of imines or ketones into a zinc hydride bond has been previously proposed and observed. 11,64,65 The aromatized zinc amido or alkoxy complex, per the stoichiometric experiments, can release product across the side arm via MLC (through intermediate F), regenerating the dearomatized zinc methyl complex (A and B) to propagate the cycle. It is worth noting that the zinc amido or alkoxy intermediate (E) could also undergo sigma bond metathesis with hydrogen (a more typical mechanism for a main group metal) via a more energetically demanding pathway (vide infra), which would also be a productive route to regenerate (C). 13 DFT calculations at the ωB97M-V/def2-TZVPP/RIJ-COSX/SMD//M06-L/def2-TZVP/GD3/W06/SMD level of theory were performed on the model system (X = Me; substrate = N-benzylideneaniline, 1 M standard states except H 2 7 atm) to provide insight into the plausibility of the proposed mechanism and to interrogate specifically whether product release via MLC (loss of amine from E to F to B) versus product release by hydrogenolysis (hydrogenation of E to C) is more favorable. In particular, computation indicates that the largest activation energy of the MLC pathway is the initial activation of hydrogen, which is overall 7.4 kcal/mol lower in energy than the highest energy barrier of the sigma bond metathesis pathway, which is the activation of hydrogen at the zinc amido complex (E to C; activation energy: 40.7 kcal/mol). Loss of amine via MLC has a barrier of 28.0 kcal/ mol (E to F), which is 12.7 kcal/mol lower in energy than the Journal of the American Chemical Society pubs.acs.org/JACS Article hydrogenolysis product-forming step of the alternative mechanism. This difference supports the notion that both hydrogen activation and loss of amine through the MLC pathway is substantially more favorable than splitting hydrogen by sigma bond metathesis to generate product (see Supporting Information for full computational details).
To further probe these possible mechanisms, we also performed the hydrogenation experiments with zinc alkyl and amido species without the PNP tBu ligand, which would be unable to proceed by a MLC pathway. Dimethylzinc alone shows no activity for imine hydrogenation under the standard conditions. Zinc bis(trimethylsilyl)amide, however, showed some activity across several experimental trials; 16 however, a mercury test suppressed much of its activity for imine hydrogenation, and several trials of the same conditions led to variant results, leading us to believe that this activity is heterogeneous. Supporting this hypothesis, under the ketone hydrogenation conditions, zinc bis(trimethylsilyl)amide alone again gave varying results, and additionally suffers from selectivity problems (see Supporting Information). On the contrary, the presence of mercury had limited to no effect on the activity of 1 for both imine and ketone hydrogenation. Nonetheless, considering these computational and experimental findings, a contribution of the sigma bond metathesis pathway is unlikely but possible, and in addition, we cannot rule out other possible outer sphere mechanisms or an FLPlike mechanism involving the labile arm, which was recently reported for a copper pincer complex. 66 In that respect, it is interesting to note that the proposed pathway does not specifically implicate the labile arm, indicating that PN complexes may also be suitable for such transformations. 43,67 Finally, with respect to the resting state and active catalytic species, we also note that during the course of the catalytic reaction, the zinc methyl moiety (denoted X in Figure 4) may be protonated with product (supported by the observation of the proposed complex, PNP tBu *ZnNPhBn, in the equilibrium described above), especially as the concentration of amine or alcohol increases during the reaction. This substitution may or may not enhance the catalytic activity of the system. Indeed, monitoring the hydrogenation of 5 equiv of N-benzylideneaniline in an NMR tube with 5 bar of hydrogen, in addition to free amine product, during the reaction we observed 1 with bound amine (6) and 7 in equilibrium as the major species, but also a species that may be the activation of the free imine across the side arm which forms initially (maximum observed concentration ca. 30%) and then decays as hydrogenation proceeds (depicted as G, but may be one of several isomers; see Supporting Information) 68 and observable amounts of PNP tBu *ZnNPhBn. Therefore, this finding, in conjunction with the aforementioned equilibrium experiment and Zn−H trapping experiment (outlined in Scheme 2), suggests that the formation of PNP tBu *ZnNPhBn depends on the ratio of free amine to zinc complex in the system. We hypothesized that PNP tBu *ZnNPhBn is likely also catalytically competent. In accordance, complex 4, prepared in situ from 3 and NaN(SiMe 3 ) 2 , is also active for imine and ketone hydrogenation. Regardless of the X substitution, in agreement with the computation, activation of hydrogen via MLC is likely the rate-determining step of the catalytic cycle. Further supporting this notion, we observe an approximate kinetic isotope effect of 1.71 when the model imine hydrogenation is performed in a high-pressure NMR tube with a mixture of H 2 and D 2 (see Supporting Information).

■ CONCLUSION
In conclusion, a series of dearomatized zinc pincer complexes supported by the PNP tBu ligand were prepared and characterized. The reactivity of PNP tBu *ZnMe was explored, allowing for the unique observation of reversible N−H and H− H bond activation by MLC by a main group metal complex. Mechanistic studies indicate that hemilability of the phosphorus arms is key in allowing for this novel bond activation by zinc. Utilizing this zinc pincer system in catalysis, imines and ketones have been hydrogenated via a mechanism in which aromatization/dearomatization MLC was found to play a role in key steps of the catalytic cycle: H 2 activation and product release. Thus, leveraging MLC shows significant promise in advancing main group metal (de)hydrogenation catalysis. The study of further bond activations and catalytic applications of this system is currently underway, with the aim of broadening the capabilities of main group catalysts.