Replacing the -phenyl Ring in Tamoxifen with a -Connected NCN Pincer-Pt-Cl Grouping by Post-Modification †.

Post-modification of a series of NCN-pincer platinum(II) complexes [PtX(NCN-R-4)] (NCN = [CH(CHNMe)-2,6], R = C(O)H, C(O)Me and C(O)Et), X = Cl or Br) at the -position using the McMurry reaction was studied. The synthetic route towards two new [PtCl(NCN-R-4)] (R = C(O)Me and C(O)Et) complexes used above is likewise described. The utility and limitations of the McMurry reaction involving these pincer complexes was systematically evaluated. The predicted "homo-coupling" reaction of [PtBr(NCN-C(O)H-4)] led to the unexpected formation of 3,3',5,5'-tetra[(dimethylamino)methyl]-4,4'-bis(platinum halide)-benzophenone (halide = Br or Cl), referred to hereafter as the bispincer-benzophenone complex . This material was further characterized using X-ray crystal structure determination. The applicability of the pincer complexes in the McMurry reaction is shown to open a route towards the synthesis of tamoxifen-type derivatives of which one phenyl ring of Tamoxifen itself is replaced by an NCN arylplatinum pincer fragment. The newly synthesized derivatives can be used as potential candidates in anti-cancer drug screening protocols. Two NCN-arylpincer platinum tamoxifen type derivatives, and , were successfully synthesized and of the separation of the diastereomeric -forms was achieved. Compound , which is the pivaloyl protected NCN pincer platinum hydroxy-Tamoxifen derivative, was obtained as a mixture of isomers. The new derivatives were further analyzed and characterized with H-, C{H}- and Pt{H}-NMR, IR, exact mass MS and elemental analysis.