TY - JOUR
T1 - Cationic, linear Au(I) N-heterocyclic carbene complexes: synthesis, structure and anti-mitochondrial activity
AU - Baker, Murray
AU - Barnard, Peter
AU - Berners-Price, Susan
AU - Brayshaw, S.K.
AU - Hickey, J.L.
AU - Skelton, Brian
AU - White, Allan
PY - 2006
Y1 - 2006
N2 - Six linear, two-coordinate cationic Au( I) N-heterocyclic carbene complexes of the form [(R(2)Im)(2)Au](+) (R = Me 1, Me, Et 2, i-Pr 3, n-Bu 4, t-Bu 5 and Cy 6) have been prepared by the reaction of two equivalents of the appropriate dialkylimidazol-2-ylidene (R(2)Im) with (Me2S) AuCl in dmf. Single crystal structural studies for 1 . PF6, 2 . PF6, 3 . Cl and 4 - 6 . PF6 show that for all six complexes the gold( I) centres have quasi-linear C - Au - C coordination, with quasi-parallel pairs of aromatic imidazole planes, except in 5 . PF6 where they are quasi- normal; in the latter, Au - C are 2.038( 3), 2.033( 3) angstrom, cf. ( e. g.) 3 2.027( 2) angstrom. Inter-cation Au center dot center dot center dot Au are close at 3.487( 2), 3.525( 2) angstrom in 1 . PF6 and 2 . PF6. The structural studies and low temperature NMR experiments provide no supportive evidence for the presence of pi back-bonding within this series of complexes. The lipophilicities of the six compounds, as estimated from the logarithm of the n-octanol-water partition coefficients ( log P), varied across the series within the range - 1.09 to 1.73. To investigate their potential as possible anti-mitochondrial anti-tumour agents, five of the compounds have been evaluated for their propensities to induce mitochondrial membrane permeabilization (MMP) in isolated rat liver mitochondria. At concentrations between 1 - 10 mu M compounds 1 . Br and 3 - 6 . Cl induced dose-dependent, Ca2+-sensitive mitochondrial swelling at rates that increased with the lipophilicities of the complexes, with the most lipophilic compounds inducing the most rapid onset of swelling. The swelling was completely inhibited by cyclosporin A, the specific inhibitor of the mitochondrial permeability transition pore.
AB - Six linear, two-coordinate cationic Au( I) N-heterocyclic carbene complexes of the form [(R(2)Im)(2)Au](+) (R = Me 1, Me, Et 2, i-Pr 3, n-Bu 4, t-Bu 5 and Cy 6) have been prepared by the reaction of two equivalents of the appropriate dialkylimidazol-2-ylidene (R(2)Im) with (Me2S) AuCl in dmf. Single crystal structural studies for 1 . PF6, 2 . PF6, 3 . Cl and 4 - 6 . PF6 show that for all six complexes the gold( I) centres have quasi-linear C - Au - C coordination, with quasi-parallel pairs of aromatic imidazole planes, except in 5 . PF6 where they are quasi- normal; in the latter, Au - C are 2.038( 3), 2.033( 3) angstrom, cf. ( e. g.) 3 2.027( 2) angstrom. Inter-cation Au center dot center dot center dot Au are close at 3.487( 2), 3.525( 2) angstrom in 1 . PF6 and 2 . PF6. The structural studies and low temperature NMR experiments provide no supportive evidence for the presence of pi back-bonding within this series of complexes. The lipophilicities of the six compounds, as estimated from the logarithm of the n-octanol-water partition coefficients ( log P), varied across the series within the range - 1.09 to 1.73. To investigate their potential as possible anti-mitochondrial anti-tumour agents, five of the compounds have been evaluated for their propensities to induce mitochondrial membrane permeabilization (MMP) in isolated rat liver mitochondria. At concentrations between 1 - 10 mu M compounds 1 . Br and 3 - 6 . Cl induced dose-dependent, Ca2+-sensitive mitochondrial swelling at rates that increased with the lipophilicities of the complexes, with the most lipophilic compounds inducing the most rapid onset of swelling. The swelling was completely inhibited by cyclosporin A, the specific inhibitor of the mitochondrial permeability transition pore.
U2 - 10.1039/b602560a
DO - 10.1039/b602560a
M3 - Article
C2 - 16865184
SN - 1477-9226
VL - 2006
SP - 3708
EP - 3715
JO - Dalton Transactions
JF - Dalton Transactions
IS - 30
ER -