High-resolution EPR spectroscopic investigations of a homologous set of d9-cobalt(0), d9-rhodium(0), and d9-iridium(0) complexes.

The 17-electron complexes [M(tropp(ph))2] (M=Co0, Rh0, Ir0) were prepared and isolated (tropp = tropylidene phosphane). A structural analysis of [Co(tropp(ph))2] revealed this complex to be almost tetrahedral, while the heavier homologues have more planar structures. Partially deuterated tropp complexes [D6][M(tropp(ph))2] were synthesised for M = Rh and Ir in order to enhance the resolution in the EPR spectra. This synthesis involves a four-fold intramolecular C-H activation reaction, whereby alkyl groups are transformed into olefins. Dihydrides were observed as intermediates for M = Ir. The electronic and geometric structures of all complexes [M(tropp(ph))2] (M = Co, Rh, Ir) and [D6][M(tropp(ph))2] (M = Rh, Ir) were investigated by continuous wave (CW) and echo-detected EPR in combination with pulse ENDOR and ESEEM techniques. In accord with their planar structures, cis and trans isomers were detected for [M(tropp(ph))2] (M = Rh0, Ir0) for which a dynamic equilibrium was established. The thermodynamic data show that the cis isomer is slightly preferred by deltaH(o) = -4.7 +/- 0.3 kJ mol(-1) (M = Rh) and delta H(o) = -5.1 +/- 0.5 kJ mol(-1); (M = Ir). The entropies for the process trans-[M(tropp(ph))2] <==> cis-[M(tropp(ph))2] are also negative [deltaS(o) = -5 +/- 1.5 J mol(-1) (M = Rh); deltaS(o) = -17 +/- 3.7 J mol(-1) (M = Rh)], indicating higher steric congestion in the cis isomers. The cobalt(0) and irdium(0) complexes show rather large g anisotropies, while that of the rhodium(0) complex is small (Co: g(parallel) = 2.320, g(perpendicular) = 2.080; cis-Rh: g(parallel) = 2.030, g(perpendicular) = 2.0135; trans-Rh: g(parallel) = 2.050, g(perpendicular) = 2.030; cis-Ir: g(parallel) = 2.030, g(perpendicular) = 2.060; trans-Ir: g(parallel) = 1.980, g(perpendicular) = 2.150). The g matrices of [M(tropp(ph))2] (M = Co, Rh) are axially symmetric with g(parallel) > g(perpendicular), indicating either a distorted square planar structure (SOMO essentially d(x2 - y2) or a compressed tetrahedron (SOMO essentially d(xy)). Interestingly, for [Ir(tropp(ph))2] the inverse ordering, g(perpendicular) > g(parallel) is found; this cannot be explained by simple ligand field arguments and must await a more sophisticated analysis. The hyperfine interactions of the unpaired electron with the metal nuclei, phosphorus nuclei, protons, deuterons and carbon nuclei were determined. By comparison with atomic constants, the spin densities on these centres were estimated and found to be small. However, the good agreement of the distance between the olefinic protons and the metal centres determined from the dipolar coupling parameter indicates that the unpaired electron is primarily located at the metal centre

Single Rapamycin Administration Induces Prolonged Downward Shift in Defended Body Weight in Rats

Manipulation of body weight set point may be an effective weight loss and maintenance strategy as the homeostatic mechanism governing energy balance remains intact even in obese conditions and counters the effort to lose weight. However, how the set point is determined is not well understood. We show that a single injection of rapamycin (RAP), an mTOR inhibitor, is sufficient to shift the set point in rats. Intraperitoneal RAP decreased food intake and daily weight gain for several days, but surprisingly, there was also a long-term reduction in body weight which lasted at least 10 weeks without additional RAP injection. These effects were not due to malaise or glucose intolerance. Two RAP administrations with a two week interval had additive effects on body weight without desensitization and significantly reduced the white adipose tissue weight. When challenged with food deprivation, vehicle and RAP-treated rats responded with rebound hyperphagia, suggesting that RAP was not inhibiting compensatory responses to weight loss. Instead, RAP animals defended a lower body weight achieved after RAP treatment. Decreased food intake and body weight were also seen with intracerebroventricular injection of RAP, indicating that the RAP effect is at least partially mediated by the brain. In summary, we found a novel effect of RAP that maintains lower body weight by shifting the set point long-term. Thus, RAP and related compounds may be unique tools to investigate the mechanisms by which the defended level of body weight is determined; such compounds may also be used to complement weight loss strategy