Donor-activated alkali metal dipyridylamides: co-complexation reactions with zinc alkyls and reactivity studies with benzophenone.

Previously it was reported that activation of (t)Bu2Zn by [(TMEDA)Na(μ-dpa)]2 led to tert-butylation of benzophenone at the challenging para-position, where the sodium amide functions as a metalloligand towards (t)Bu2Zn manifested in crystalline [{(TMEDA)Na(dpa)}2Zn(t)Bu2] (TMEDA is N,N,N',N'-tetramethylethylenediamine, dpa is 2,2'-dipyridylamide). Here we find altering the Lewis donor or alkali metal within the metalloligand dictates the reaction outcome, exhibiting a strong influence on alkylation yields and reaction selectivity. Varying the former led to the synthesis of three novel complexes, [(PMDETA)Na(dpa)]2, [(TMDAE)Na(dpa)]2, and [(H6-TREN)Na(dpa)], characterised through combined structural, spectroscopic and theoretical studies [where PMDETA is N,N,N',N'',N''-pentamethyldiethylenetriamine, TMDAE is N,N,N',N'-tetramethyldiaminoethylether and H6-TREN is N',N'-bis(2-aminoethyl)ethane-1,2-diamine]. Each new sodium amide can function as a metalloligand to generate a co-complex with (t)Bu2Zn. Reacting these new co-complexes with benzophenone proved solvent dependent with yields in THF much lower than those in hexane. Most interestingly, sub-stoichiometric amounts of the metalloligands [(TMEDA)Na(dpa)]2 and [(PMEDTA)Na(dpa)]2 with 1 : 1, (t)Bu2Zn-benzophenone mixtures produced good yields of the challenging 1,6-tert-butyl addition product in hexane (52% and 53% respectively). Although exchanging Na for Li gave similar reaction yields, the regioselectivity was significantly compromised; whereas the K system was completely unreactive. Replacing (t)Bu2Zn with (Me3SiCH2)2Zn shut down the alkylation of benzophenone; in contrast, (t)BuLi generates only the reduction product, benzhydrol. Zincation of the parent amine dpa(H) generated the crystalline product [Zn(dpa)2], as structurally elucidated through X-ray crystallography and theoretical calculations. Although the reaction mechanism for the alkylation of benzophenone remains unclear, incorporation of the radical scavenger TEMPO (2,2,6,6-tetramethylpiperidine-N-oxyl radical) into the reaction system completely inhibits benzophenone alkylation.