om0492350_si_006.cif (29.94 kB)
Synthesis and Structure of Group 4 Iminophosphonamide Complexes
dataset
posted on 2005-02-14, 00:00 authored by Rainer Vollmerhaus, Robert Tomaszewski, Pengcheng Shao, Nicholas J. Taylor, Kevin J. Wiacek, Stewart P. Lewis, Abdulaziz Al-Humydi, Scott CollinsThe syntheses of a variety of iminophosphonamide (PN2) ligands (2a−f), the corresponding
hydrochloride salts (1a−c), and a number of bis(PN2) dichloride complexes of group 4 (3a−e) and their corresponding dialkyls (5a−e) are described. A novel monosubstituted PN2 “ate”
complex 4 was prepared from ligand 2f and Zr(NMe2)4 on treatment with excess Me2NH·HCl. Piano-stool PN2 zirconium dichloride complexes 6a−h were accessible on treatment of
CpZr(NMe2)3 (Cp = C5H5, Cp*) with PN2 ligands 2a−e, followed by metathesis with excess
Me3SiCl or Me2NH·HCl (6a−g) or at low T with ethereal HCl (6h). Dialkyl derivatives 8a−h
could be prepared from 6a−h or directly from ligands 2 and CpMMe3 (Cp = C5H5, Cp*; M
= Ti or Zr). The intermediate Cp(PN2)Zr(NMe2)2, precursor to 6h, rearranged to the novel
terminal difluoride complexes 7a,b at room temperature. A variety of complexes 3 and 6 or
their corresponding alkyl derivatives have been characterized by X-ray crystallography. In
addition, the novel “ate” complex 4 and difluoride complexes 7a,b have been structurally
characterized in this manner. The structures of 7a,b in the solid state reveal strong,
intramolecular coordination of the NMe2 group to the metal center, resulting in eight-coordinate complexes. One of these complexes is fluxional in solution, suggesting rapid
exchange of bound versus free NMe2 groups coupled with the formation of coordination
stereoisomers.